GAMMA POLYGLUTAMATED PRALATREXATE AND USES THEREOF

Title:

GAMMA POLYGLUTAMATED PRALATREXATE AND USES THEREOF

Document Type and Number:

WIPO Patent Application WO/2019/160736

Kind Code:

Abstract:

The disclosure relates generally to gamma polyglutamated pralatrexate compositions, including delivery vehicles such as liposomes containing the gamma polyglutamated pralatrexate, and methods of making and using the gamma polyglutamated pralatrexate compositions to treat hyperproliferative disorders (e.g., cancer) and disorders of the immune system (e.g., inflammation and autoimmune diseases such as rheumatoid arthritis).

Inventors:

NIYIKIZA CLET (US)
MOYO VICTOR (US)

Application Number:

PCT/US2019/016981

Publication Date:

August 22, 2019

Filing Date:

February 07, 2019

Export Citation:

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Assignee:

L E A F HOLDINGS GROUP LLC (US)

International Classes:

A61K31/519; C07D475/04; C07K16/28

Foreign References:

US7446120B2	2008-11-04
US9440979B2	2016-09-13

Other References:

VISENTIN ET AL.: "The Antifolates", HEMATOL ONCOL CLIN NORTH AM., vol. 26, no. 3, 2012, pages 629, XP055631097, ISSN: 0889-8588, DOI: 10.1016/j.hoc.2012.02.002
TOMSHO ET AL.: "Concentration-Dependent Processivity of Multiple Glutamate Ligations Catalyzed by Folylpoly-gamma-glutamate Synthetase", BIOCHEMISTRY, vol. 47, no. 34, 2008, pages 9040 - 9050, XP055629157
See also references of EP 3752156A4

Attorney, Agent or Firm:

HOOVER, Kenley, K. (US)

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Claims:

WHAT IS CLAIMED IS:

1. A composition comprising a gamma polyglutamated pralatrexate.

2. The composition of claim 1, wherein the gamma polyglutamated pralatrexate comprises 1-10 glutamyl groups having gamma carboxyl group linkages.

3. The composition of claim 1 or 2, wherein the gamma polyglutamated pralatrexate contains 4, 5, 2-10, 4-6, or more than 5, glutamyl groups having gamma carboxyl group linkages.

4. The composition according to any of claims 1-3, wherein the gamma

polyglutamated pralatrexate is gamma tetraglutamated pralatrexate.

5. The composition according to any of claims 1-3, wherein the gamma

polyglutamated pralatrexate is gamma pentaglutamated pralatrexate.

6. The composition according to any of claims 1-3, wherein the gamma

polyglutamated pralatrexate is gamma hexaglutamated pralatrexate.

7. The composition according to any of claims 1-6, wherein

(a) the gamma polyglutamated pralatrexate comprises two or more glutamyl groups in the L-form having gamma carboxyl group linkages,

(b) each of the glutamyl groups of the gamma polyglutamated pralatrexate is in the L-form and has a gamma carboxyl group linkage,

(c) at least one of the glutamyl groups of the gamma polyglutamated pralatrexate is in the D- form and has a gamma carboxyl group linkage,

(d) each of the glutamyl groups of the gamma polyglutamated pralatrexate other than the glutamyl group of pralatrexate is in the D-form and has a gamma carboxyl group linkage, or

(e) the gamma polyglutamated pralatrexate comprises two or more glutamyl groups in the L-form and at least one glutamyl group in the D-form having gamma carboxyl group linkages.

8. The composition according to 4, wherein (a) each of the glutamyl groups is in the L-form and has a gamma carboxyl group linkage or (b) each of the glutamyl groups other than the glutamyl group of pralatrexate is in the D-form and and each of the gluytamyl groups has a gamma carboxyl group linkage.

9. The composition of claim 5, wherein (a) each of the glutamyl groups is in the L- form and has a gamma carboxyl group linkage or (b) each of the glutamyl groups other than the glutamyl group of pralatrexate is in the D-form and and each of the gluytamyl groups has a gamma carboxyl group linkage.

10. The composition of claim 6, wherein (a) each of the glutamyl groups is in the L- form and has a gamma carboxyl group linkage or (b) each of the glutamyl groups other than the glutamyl group of pralatrexate is in the D-form and and each of the gluytamyl groups has a gamma carboxyl group linkage.

11. The composition according to any of claims 1-10, wherein the gamma polyglutamated pralatrexate is polyglutamable by FGPS under standard operating conditions,

12. A liposomal composition comprising the gamma polyglutamated pralatrexate according to any of claims 1-11 (Lp-gRRTC).

13. The Lp-gRRTC composition according to 12, wherein the gamma polyglutamated pralatrexate comprises two or more glutamyl groups in the L-form.

14. The Lp-gRRTC composition according to 12 or 13, wherein each of the glutamyl groups of the gamma polyglutamated pralatrexate is in the L-form.

15. The Lp-gRRTC composition of claim 12 or 13, wherein at least one of the glutamyl groups of the gamma polyglutamated pralatrexate is in the D-form.

16. The Lp-gRRTC composition according to any of claims 12-15, wherein the liposome comprises a gamma polyglutamated pralatrexate comprising 1-10 glutamyl groups having gamma carboxyl group linkages.

17. The Lp-gRRTC composition according to any of claims 12-16, wherein the liposome comprises a gamma polyglutamated pralatrexate containing 4, 5, 2-10, 4-6, or more than 5, glutamyl groups.

18. The Lp-gRRTC composition according to any of claims 12-17, wherein the liposome comprises gamma tetraglutamated pralatrexate.

19. The Lp-gRRTC composition according to any of claims 12-17, wherein the liposome comprises gamma pentaglutamated pralatrexate.

20. The Lp-gRRTC composition according to any of claims 12-17, wherein the liposome comprises gamma hexaglutamated pralatrexate.

21. The Lp-gRRTC composition according to any of claims 12-20, wherein the liposome is not pegylated (PyLp-yPPTX).

22. The Lp-gRRTC composition according to any of claims 12-20, wherein the liposome is pegylated (PyLp-yPPTX).

23. The Lp-gRRTC composition according to any of claims 12-23, wherein the liposomes comprise at least 1 % weight by weight (w/w) of the gamma polyglutamated pralatrexate or wherein during the process of preparing the Lp- gRRTC, at least 1% of the starting material of gamma polyglutamated PTX is encapsulated (entrapped) in the Lp-gRRTC.

24. The Lp-gRRTC composition according to any of claims 12-24, wherein the liposome has a diameter in the range of 20 nm to 500 nm.

25. The Lp-gRRTC composition according to any of claims 12-24, wherein the liposome has a diameter in the range of 20 nm to 200 nm.

26. The Lp-gRRTC composition according to any of claims 12-25, wherein the liposome has a diameter in the range of 80 nm to 120 nm.

27. The Lp-gRRTC composition according to any of claims 12-26, wherein the liposome is formed from liposomal components.

28. The Lp-gRRTC composition according to 27, wherein the liposomal components comprise at least one of an anionic lipid and a neutral lipid.

29. The Lp-gRRTC composition according to 27 or 28, wherein the liposomal components comprise at least one selected from the group consisting of: DSPE; DSPE-PEG; DSPE-PEG-maleimide; HSPC; HSPC-PEG; cholesterol; cholesterol-PEG; and cholesterol- maleimide.

30. The Lp-gRRTC composition according to any of claims 27-29, wherein the liposomal components comprise at least one selected from the group consisting of: DSPE; DSPE-PEG; DSPE-PEG-FITC; DSPE-PEG-maleimide; cholesterol; and HSPC.

31. The Lp-gRRTC composition according to any of claims 27-30, wherein one or more liposomal components further comprises a steric stabilizer.

32. The Lp-gRRTC composition according to 31, wherein the steric stabilizer is at least one selected from the group consisting of polyethylene glycol (PEG); poly-L-lysine (PLL); monosialoganglioside (GM1); poly(vinyl pyrrolidone) (PVP); poly(acrylamide) (PAA); poly(2-methyl-2-oxazoline); poly(2-ethyl-2-oxazoline); phosphatidyl polyglycerol; poly[N-(2- hydroxypropyl) methacrylamide]; amphiphilic poly-N-vinylpyrrolidones; L-amino-acid-based polymer; oligoglycerol, copolymer containing polyethylene glycol and polypropylene oxide, Poloxamer 188, and polyvinyl alcohol.

33. The Lp-gRRTC composition according to 32, wherein the steric stabilizer is PEG and the PEG has a number average molecular weight (Mn) of 200 to 5000 daltons.

34. The Lp-gRRTC composition according to any of claims 12-33, wherein the liposome is anionic or neutral.

35. The Lp-gRRTC composition according to any of claims 12-33, wherein the liposome has a zeta potential that is less than or equal to zero.

36. The Lp-gRRTC composition according to any of claims 12-33, wherein the liposome has a zeta potential that is between 0 to -150 mV.

37. The Lp-gRRTC composition according to any of claims 12-33, wherein the liposome has a zeta potential that is between -30 to -50 mV.

38. The Lp-gRRTC composition according to any of claims 12-33, wherein the liposome is cationic.

39. The Lp-gRRTC composition according to any of claims 12-38, wherein the liposome has an interior space comprising the gamma polyglutamated pralatrexate and an aqueous pharmaceutically acceptable carrier.

40. The Lp-gRRTC composition of claim 39, wherein the pharmaceutically acceptable carrier comprises a tonicity agent such as dextrose, mannitol, glycerine, potassium chloride, sodium chloride, at a concentration of greater than 1%.

41. The Lp-gRRTC composition of claim 39, wherein the aqueous pharmaceutically acceptable carrier is trehalose.

42. The Lp-gRRTC composition of claim 41, wherein the pharmaceutically acceptable carrier comprises 1% to 50% trehalose.

43. The Lp-gRRTC composition according to any of claims 39 -42, wherein the pharmaceutically acceptable carrier comprises 1% to 50% dextrose solution.

44. The Lp-gRRTC composition according to any of claims 39-43, wherein the interior space of the liposome comprises 5% dextrose suspended in an HEPES buffered solution.

45. The Lp-gRRTC composition according to any of claims 39-44, wherein the pharmaceutically acceptable carrier comprises a buffer such as HEPES Buffered Saline (HBS) or similar, at a concentration of between 1 to 200 mM and a pH of between 2 to 8.

46. The Lp-gRRTC composition according to any of claims 39-45, wherein the pharmaceutically acceptable carrier comprises a total concentration of sodium acetate and calcium acetate of between 50 mM to 500 mM.

47. The Lp-gRRTC composition according to any of claims 12-46, wherein the interior space of the liposome has a pH of 5-8 or a pH of 6-7, or any range therein between.

48. The Lp-gRRTC composition according to any of claims 12-47, wherein the liposome comprises less than 500,000 or less than 200,000 molecules of the gamma polyglutamated pralatrexate.

49. The Lp-gRRTC composition according to any of claims 12-48, wherein the liposome comprises between 10 to 100,000 molecules of the gamma polyglutamated pralatrexate, or any range therein between.

50. The Lp-gRRTC composition according to any of claims 12-49, which further comprises a targeting moiety and wherein the targeting moiety has a specific affinity for a surface antigen on a target cell of interest.

51. The Lp-gRRTC composition according to 50, wherein the targeting moiety is attached to one or both of a PEG and the exterior of the liposome, optionally wherein targeting moiety is attached to one or both of the PEG and the exterior of the liposome by a covalent bond.

52. The Lp-gRRTC composition of claim 50 or 51, wherein the targeting moiety is a polypeptide.

53. The Lp-gRRTC composition according to any of claims 50-52, wherein the targeting moiety is an antibody or an antigen binding fragment of an antibody.

54. The Lp-gRRTC composition according to any of claims 50-53, wherein the targeting moiety binds the surface antigen with an equilibrium dissociation constant (Kd) in a range of 0.5 x 10 ¹⁰ to 10 x 10⁶ as determined using BIACORE®analysis.

55. The Lp-gRRTC composition according to any of claims 50-54, wherein the targeting moiety specifically binds one or more folate receptors selected from the group consisting of: folate receptor alpha (FR-a), folate receptor beta (FR-b), and folate receptor delta (FR-d).

56. The Lp-gRRTC composition according to any of claims 50-55, wherein the targeting moiety comprises one or more selected from the group consisting of: an antibody, a humanized antibody, an antigen binding fragment of an antibody, a single chain antibody, a single-domain antibody, a bi-specific antibody, a synthetic antibody, a pegylated antibody, and a multimeric antibody.

57. The Lp-gRRTC composition according to any of claims 50-56, wherein each pegylated liposome comprises from 1 to 1000 or 30-200 targeting moieties.

58. The Lp-gRRTC composition according to any of claims 39-57, further comprising one or more of an immunostimulatory agent, a detectable marker and a maleimide, wherein the immunostimulatory agent, the detectable marker or the maleimide is attached to said PEG or the exterior of the liposome.

59. The Lp-gRRTC composition of claim 58, wherein the immunostimulating agent is at least one selected from the group consisting of: a protein immunostimulating agent; a nucleic acid immunostimulating agent; a chemical immunostimulating agent; a hapten; and an adjuvant.

60. The Lp-gRRTC composition of claim 58 or 59, wherein the immunostimulating agent is at least one selected from the group consisting of: a fluorescein; a fluorescein isothiocyanate (FITC); a DNP; a beta glucan; a beta-l,3-glucan; a beta-l,6-glucan; a resolvin (e.g., a Resolvin D such as D_n-6DPA or D„ -,i,_|.L, a Resolvin E, or a T series resolvin); and a Toll like receptor (TLR) modulating agent such as, an oxidized low-density lipoprotein (e.g.

OXPAC, PGPC), and an eritoran lipid (e.g., E5564).

61. The Lp-gRRTC composition according to any of claims 58-60, wherein the immunostimulatory agent and the detectable marker is the same.

62. The Lp-gRRTC composition according to any of claims 58-61, further comprising a hapten.

63. The Lp-gRRTC composition of claim 62, wherein the hapten comprises one or more of fluorescein or Beta 1, 6-glucan.

64. The Lp-gRRTC composition according to any of claims 12-63, which further comprises at least one cryoprotectant selected from the group consisting of mannitol; trehalose; sorbitol; and sucrose.

65. A targeted composition comprising the composition according to any of claims 1- 64.

66. A non-targeted composition comprising the composition according to any of claims 1-49.

67. The Lp-gRRTC composition according to any of claims 12-66, which further comprises carboplatin and/or pembroluzumab.

68. A pharmaceutical composition comprising the liposomal gamma polyglutamated pralatrexate composition according to any of claims 12-67.

69. A pharmaceutical composition comprising gamma polyglutamated pralatrexate composition according to any of claims 1-7.

70. The composition of any of claims 1-69, for use in the treatment of disease.

71. Use of the composition of any of claims 1-70, in the manufacture of a medicament for the treatment of disease.

72. A method for treating or preventing disease in a subject needing such treatment or prevention, the method comprising administering the composition of any of claims 1-70 to the subject.

73. A method for treating or preventing disease in a subject needing such treatment or prevention, the method comprising administering the liposomal gamma polyglutamated pralatrexate composition of any of claims 12-69 to the subject.

74. A method of killing a hyperproliferative cell that comprises contacting a hyperproliferative cell with the composition of any of claims 1-69].

75. A method of killing a hyperproliferative cell that comprises contacting a hyperproliferative cell with the liposomal gamma polyglutamated pralatrexate composition of any of claims 12-69.

76. The method of claim 74 or 75, wherein the hyperproliferative cell is a cancer cell, a mammalian cell, and/or a human cell.

77. A method for treating cancer that comprises administering an effective amount of the composition of any of claims 1-69 to a subject having or at risk of having cancer.

78. A method for treating cancer that comprises administering an effective amount of the liposomal gamma polyglutamated pralatrexate composition of any of claims 12-68 to a subject having or at risk of having cancer.

79. The method of claim 77 or 78, wherein the cancer is selected from the group consisting of: a non-hematologic malignancy including such as for example, lung cancer, pancreatic cancer, breast cancer, ovarian cancer, prostate cancer, head and neck cancer, gastric cancer, gastrointestinal cancer, colorectal cancer, esophageal cancer, cervical cancer, liver cancer, kidney cancer, biliary duct cancer, gallbladder cancer, bladder cancer, sarcoma (e.g., osteosarcoma), brain cancer, central nervous system cancer, and melanoma; and a hematologic malignancy such as for example, a leukemia, a lymphoma and other B cell malignancies, myeloma and other plasma cell dyscrasias.

80. The method of claim 77 or 78, wherein the cancer is a member selected from the group consisting of: wherein the cancer is a member selected from the group consisting of: lung cancer, breast cancer, colon cancer, pancreatic cancer, gastric cancer, bladder cancer, head and neck cancer, ovarian cancer, cervical cancer, cancer of the fallopian tubes, and a primary peritoneal cancer.

81. The method of claim 77 or 78, wherein the cancer is mesothelioma or non-small cell lung carcinoma (NSCLC).

82. The method of claim 77 or 78, wherein the cancer is a lymphoma, such as a T- cell lymphoma (e.g., refractory peripheral T-cell lymphoma (PTCL).

83. A method for treating cancer that comprises administering an effective amount of the Lp-gRRTC composition of any of claims 50-66 to a subject having or at risk of having a cancer cell that expresses on its surface a folate receptor bound by the targeting moiety.

84. A maintenance therapy for subjects that are undergoing or have undergone cancer therapy that comprise administering an effective amount of the composition of any of claims 1- 69 to a subject that is undergoing or has undergone cancer therapy.

85. A maintenance therapy for subjects that are undergoing or have undergone cancer therapy that comprise administering an effective amount of the liposomal gamma

polyglutamated pralatrexate composition of any of claims 12-69 to a subject that is undergoing or has undergone cancer therapy.

86. A method for treating a disorder of the immune system that comprises administering an effective amount of the composition of any of claims 1-69 to a subject having or at risk of having a disorder of the immune system.

87. A method for treating a disorder of the immune system that comprises administering an effective amount of the liposomal gamma polyglutamated pralatrexate composition of any of claims 8-69 to a subject having or at risk of having a disorder of the immune system.

88. A method for treating an infectious disease that comprises administering an effective amount of the composition of any of claims 1-69 to a subject having or at risk of having an infectious disease.

89. A method for treating an infectious disease that comprises administering an effective amount of the liposomal gamma polyglutamated pralatrexate composition of any of claims 12-69 to a subject having or at risk of having an infectious disease.

90. A method of delivering gamma polyglutamated pralatrexate to a tumor expressing a folate receptor on its surface, the method comprising: administering the Lp- gRRTC composition of any of claims 1-69 to a subject having the tumor in an amount to deliver a therapeutically effective dose of the gamma polyglutamated pralatrexate to the tumor.

91. A method of preparing a gamma polyglutamated pralatrexate composition comprising the liposomal gamma polyglutamated pralatrexate composition of any of claims 12- 69, the method comprising: forming a mixture comprising: liposomal components and gamma polyglutamated antifolate in solution; homogenizing the mixture to form liposomes in the solution; and processing the mixture to form liposomes containing gamma polyglutamated pralatrexate.

92. A method of preparing the composition of any of claims 12-69 comprising the steps of: forming a mixture comprising: liposomal components and gamma polyglutamated pralatrexate in a solution; homogenizing the mixture to form liposomes in the solution;

processing the mixture to form liposomes entrapping and/or encapsulating gamma

polyglutamated pralatrexate; and providing a targeting moiety on a surface of the liposomes, the targeting moiety having specific affinity for at least one of folate receptor alpha (FR-a), folate receptor beta (FR-b) and folate receptor delta (FR-d).

93. The method according to claim 92, wherein the processing step includes one or more steps of: thin film hydration, extrusion, in-line mixing, ethanol injection technique, freezing-and-thawing technique, reverse-phase evaporation, dynamic high pressure

microfluidization, microfluidic mixing, double emulsion, freeze-dried double emulsion, 3D printing, membrane contactor method, and stirring.

94. The method according to claim 92, wherein said processing step includes one or more steps of modifying the size of the liposomes by one or more of steps of extrusion, high- pressure microfluidization, and/or sonication

Description:

GAMMA POLYGLUTAMATED

PRALATREXATE AND USES THEREOF

BACKGROUND

[0001] This disclosure generally relates to gamma polyglutamated pralatrexate compositions, including delivery vehicles such as liposomes containing the gamma polyglutamated pralatrexate compositions, and methods of making and using the compositions to treat diseases including hyperproliferative diseases such as cancer, disorders of the immune system such as inflammation and inflammation and rheumatoid arthritis, and infectious disease such as HIV and malaria.

[0002] Pralatrexate pralatrexate ((2S)-2-[[4-[(lRS)-l-[(2, 4-diaminopteridin-6- yl)methyl]but-3ynyl]benzoyl]amino]pentanedioic acid) is a folate analog that is the antineoplastic active agent in in products marketed under the trade name FOLOTYN® (pralatrexate injection). Pralatrexate is a 1:1 racemic mixture of S- and R- diastereomers at the CIO position (indicated with * in the Figure above). The molecular formula is C23H23N7O5 and the molecular weight is 477.48 g/mol. The structural of pralate is as follows:

[0003] FOLOTYN is indicated for the treatment of patients with relapsed or refractory peripheral T-cell lymphoma (PTCL). Pralatrexate is also an active agent in non small cell lung cancer and gynecologic cancers such as ovarian cancer, cancer of the fallopian tumes and primary peritoneal cancer.

[0004] Pralatrexate is a 10-deazaaminopterin analog of methotrexate, and is a small- molecule inhibitor of DHFR. Pralatrexate differs from methotrexate at position 10 where a carbon with a propargyl side chain is substituted for the nitrogen with a methyl substituent. This minor structural alteration results in the ability of PTX to inhibit the active catalytic site of dihydrofolate reductase (DHFR) which catalyzes the production of tetrahydrofolate (THF) from dihydrofolate (DHF). Consequently, pralatrexate interferes with the synthesis of tetrahydrofolate (THF), which serves as the primary one-carbon carrier for enzymatic processes involved in de novo synthesis of thymidylate, purine nucleotides, and the amino acids serine and methionine. The inhibition of these metabolic processes disrupt the formation of DNA, RNA, and key cellular proteins.

[0005] Folate is an essential cofactor that mediates the transfer of one-carbon units involved in nucleotide biosynthesis and DNA repair, the remethylation of homocysteine (Hey), and the methylation of DNA, proteins, and lipids. The only circulating forms of folates in the blood are monoglutamates and folate monoglutamates are the only form of folate that is transported across the cell membrane - likewise, the monoglutamate form of polyglutamatable antifolates such as pralatrexate, are transported across the cell membrane. Once taken up into cells, intracellular folate is converted to polyglutamates by the enzyme folylpoly-gamma-glutamate synthetase (FPGS).

[0006] Pralatrexate is transported into cells by the reduced folate carrier (RFC) system and folate receptors (FRs) a and b and by Proton Coupled Folate Transporter (PCFT) that is generally most active in a lower pH environment. RFC is the main transporter of pralatrexate at physiologic pH and is ubiquitously expressed in both normal and diseased cells. Pralatrexate was rationally designed for improved cellular transport via RFC-l, and to have greater intracellular drug retention through the enhanced formation of polyglutamylated conjugates. The relative difference in polyglutamate formation in normal versus malignant cells may account for the enhanced pharmacodynamic activity of pralatrexate. Pralatrexate is thought to exert its pharmacological effect primarily through inhibition of DHFR, having an IC50 in the picomolar range. Consequently, pralatrexate treatment often suffers from the dose-limiting toxicity that is a major obstacle in cancer chemotherapy. Once inside the cell, pralatrexate is polyglutamated by FPGS, which may add up to 6 L glutamyl groups in a L-gamma carboxyl group linkage to the pralatrexate. The L-gamma polyglutamation of pralatrexate by FPGS serves at least 2 main therapeutic purposes: (1) it greatly enhances pralatrexate affinity and inhibitory activity for DHFR; and (2) it facilitates the accumulation of polyglutamated pralatrexate, which unlike pralatrexate (monoglutamate), is not easily transported out of cells by cell efflux pumps. [0007] While targeting folate metabolism and nucleotide biosynthesis is a well established therapeutic strategy for cancer, for PTX, clinical efficacy is limited by a lack of tumor selectivity and the presence of de novo and acquired drug resistance. Like other antifolates, pralatrexate acts during DNA and RNA synthesis, and consequently has a greater toxic effect on rapidly dividing cells such as malignant and myeloid cells. Myelosuppression is typically the dose-limiting toxicity of pralatrexate therapy and has limited the clinical applications of pralatrexate.

[0008] Resistance to antifolates therapies like pralatrexate is typically associated with one or more of, (a) increased cell efflux pump activity, (b) decreased transport of PTX into cells (c) increased DHFR activity, (d) decreased folypolyl-gamma-glutamate synthetase (FPGS) activity, and (e) increased gamma-glutamyl hydrolase (GGH) activity, which cleaves gamma polyglutamate chains attached to folates and antifolates.

[0009] The challenge to the longstanding (>30 years) observation that higher-level poly glutamates of various antifolates have much greater potency compared to lower-level glutamates, has been that the scientific community has relied on the intracellular FPGS mediated mechanisms to convert the lower-level glutamates to their higher-level forms. The present inventions provide the means to deliver higher-level polyglutamate forms of antifolates directly into the cell, without having to rely on the cells machinery to achieve this goal.

[0010] The provided alpha polyglutamated pralatrexate compositions deliver a strategy for overcoming the pharmacological challenges associated with the dose limiting toxicides and with treatment resistance associated with pralatrexate therapy. The provided methods deliver to cancer cells a novel alpha polyglutamated form of pralatrexate while (1) minimizing/reducing exposure to normal tissue cells, (2) optimizing/improving the cytotoxic effect of pralatrexate-based agents on cancer cells and (3) minimizing/reducing the impact of the efflux pumps, and other resistance mechanisms that limit the therapeutic efficacy of pralatrexate.

BRIEF SUMMARY

[0011] This disclosure generally relates gamma polyglutamated pralatrexate (PTX) compositions and methods of making and using the compositions to treat diseases including hyperproliferative diseases such as cancer, disorders of the immune system such as inflammation and rheumatoid arthritis, and infectious disease such as HIV and malaria.

[0012] In some embodiments, the disclosure provides:

[1] a composition comprising a gamma polyglutamated pralatrexate;

[2] the composition of [1], wherein the gamma polyglutamated pralatrexate

comprises 1-10 glutamyl groups having gamma carboxyl group linkages;

[3] the composition of [1] or [2], wherein the gamma polyglutamated pralatrexate contains 4, 5, 2-10, 4-6, or more than 5, glutamyl groups having gamma carboxyl group linkages;

[4] the composition according to any of [l]-[3], wherein the gamma polyglutamated pralatrexate is gamma tetraglutamated pralatrexate;

[5] the composition according to any of [l]-[3], wherein the gamma polyglutamated pralatrexate is gamma pentaglutamated pralatrexate;

[6] the composition according to any of [l]-[3], wherein the gamma polyglutamated pralatrexate is gamma hexaglutamated pralatrexate;

[7] the composition according to any of [l]-[6], wherein

(a) the gamma polyglutamated pralatrexate comprises two or more glutamyl groups in the L-form having gamma carboxyl group linkages,

(b) each of the glutamyl groups of the gamma polyglutamated pralatrexate is in the L-form and has a gamma carboxyl group linkage,

pralatrexate is in the D-form and has a gamma carboxyl group linkage,

(d) each of the glutamyl groups of the gamma polyglutamated pralatrexate other than the glutamyl group of pralatrexate is in the D-form and has a gamma carboxyl group linkage, or

(e) the gamma polyglutamated pralatrexate comprises two or more glutamyl groups in the L-form and at least one glutamyl group in the D-form having gamma carboxyl group linkages;

[8] the composition according to [4], wherein (a) each of the glutamyl groups is in the L-form and has a gamma carboxyl group linkage or (b) each of the glutamyl groups other than the glutamyl group of pralatrexate is in the D-form and and each of the gluytamyl groups has a gamma carboxyl group linkage; [9] the composition of [5], wherein (a) each of the glutamyl groups is in the L-form and has a gamma carboxyl group linkage or (b) each of the glutamyl groups other than the glutamyl group of pralatrexate is in the D-form and and each of the gluytamyl groups has a gamma carboxyl group linkage;

[10] the composition of [6], wherein (a) each of the glutamyl groups is in the L-form and has a gamma carboxyl group linkage or (b) each of the glutamyl groups other than the glutamyl group of pralatrexate is in the D-form and and each of the gluytamyl groups has a gamma carboxyl group linkage;

[11] the composition according to any of [1]-[10], wherein the gamma polyglutamated pralatrexate is polyglutamable by FGPS under physiological conditions;

[12] a liposomal composition comprising the gamma polyglutamated pralatrexate according to any of [l]-[l l] (Lp-gRRTC);

[13] the Lp-gRRTC composition according to [12], wherein the gamma

polyglutamated pralatrexate comprises two or more glutamyl groups in the L- form;

[14] the Lp-gRRTC composition according to [12] or [13], wherein each of the

glutamyl groups of the gamma polyglutamated pralatrexate is in the L-form;

[15] the Lp-gRRTC composition of [12] or [13], wherein at least one of the glutamyl groups of the gamma polyglutamated pralatrexate is in the D-form;

[16] the Lp-gRRTC composition according to any of [12]-[15], wherein the liposome comprises a gamma polyglutamated pralatrexate comprising 1-10 glutamyl groups having gamma carboxyl group linkages;

[17] the Lp-gRRTC composition according to any of [12]-[16], wherein the liposome comprises a gamma polyglutamated pralatrexate containing 4, 5, 2-10, 4-6, or more than 5, glutamyl groups;

[18] the Lp-gRRTC composition according to any of [12]-[17], wherein the liposome comprises gamma tetraglutamated pralatrexate;

[19] the Lp-gRRTC composition according to any of [12]-[17], wherein the liposome comprises gamma pentaglutamated pralatrexate;

[20] the Lp-gRRTC composition according to any of [12]-[17], wherein the liposome comprises gamma hexaglutamated pralatrexate; [21] the Lp-gRRTC composition according to any of [l2]-[20], wherein the liposome is not pegylated (PyLp-yPPTX);

[22] the Lp-gRRTC composition according to any of [l2]-[20], wherein the liposome is pegylated (PyLp-yPPTX);

[23] the Lp-gRRTC composition according to any of [l2]-[22], wherein the liposomes comprise at least 1% weight by weight (w/w) of the gamma polyglutamated pralatrexate or wherein during the process of preparing the Lp- gRRTC, at least 1% of the starting material of gamma polyglutamated PTX is encapsulated (entrapped) in the Lp-gRRTC;

[24] the Lp-gRRTC composition according to any of [l2]-[23], wherein the liposome has a diameter in the range of 20 nm to 500 nm;

[25] the Lp-gRRTC composition according to any of [l2]-[24], wherein the liposome has a diameter in the range of 20 nm to 200 nm;

[26] the Lp-gRRTC composition according to any of [l2]-[25], wherein the liposome has a diameter in the range of 80 nm to 120 nm;

[27] the Lp-gRRTC composition according to any of [l2]-[26], wherein the liposome is formed from liposomal components;

[28] the Lp-gRRTC composition according to [27], wherein the liposomal components comprise at least one of an anionic lipid and a neutral lipid;

[29] the Lp-gRRTC composition according to [27] or [28], wherein the liposomal components comprise at least one selected from the group consisting of: DSPE; DSPE-PEG; DSPE-PEG-maleimide; HSPC; HSPC-PEG; cholesterol;

cholesterol-PEG; and cholesterol-maleimide;

[30] the Lp-gRRTC composition according to any of [27]-[29], wherein the liposomal components comprise at least one selected from the group consisting of: DSPE; DSPE-PEG; DSPE-PEG-FITC; DSPE-PEG-maleimide; cholesterol; and HSPC;

[31] the Lp-gRRTC composition according to any of [27] -[30], wherein one or more liposomal components further comprises a steric stabilizer;

[32] the Lp-gRRTC composition according to [31], wherein the steric stabilizer is at least one selected from the group consisting of polyethylene glycol (PEG); poly- L-lysine (PLL); monosialoganglioside (GM1); poly(vinyl pyrrolidone) (PVP); poly (acrylamide) (PAA); poly(2-methyl-2-oxazoline); poly(2-ethyl-2-oxazoline); phosphatidyl polyglycerol; poly[N-(2-hydroxypropyl) methacrylamide];

amphiphilic poly-N-vinylpyrrolidones; L-amino-acid-based polymer;

oligoglycerol, copolymer containing polyethylene glycol and polypropylene oxide, Poloxamer 188, and polyvinyl alcohol;

[33] the Lp-gRRTC composition according to [32], wherein the steric stabilizer is PEG and the PEG has a number average molecular weight (Mn) of 200 to 5000 daltons;

[34] the Lp-gRRTC composition according to any of [l2]-[33], wherein the liposome is anionic or neutral;

[35] the Lp-gRRTC composition according to any of [l2]-[33], wherein the liposome has a zeta potential that is less than or equal to zero;

[36] the Lp-gRRTC composition according to any of [l2]-[33], wherein the liposome has a zeta potential that is between 0 to -150 mV;

[37] the Lp-gRRTC composition according to any of [l2]-[33], wherein the liposome has a zeta potential that is between -30 to -50 mV;

[38] the Lp-gRRTC composition according to any of [l2]-[33], wherein the liposome is cationic;

[39] the Lp-gRRTC composition according to any of [l2]-[38], wherein the liposome has an interior space comprising the gamma polyglutamated pralatrexate and an aqueous pharmaceutically acceptable carrier;

[40] the Lp-gRRTC composition of [39], wherein the pharmaceutically acceptable carrier comprises a tonicity agent such as dextrose, mannitol, glycerine, potassium chloride, sodium chloride, at a concentration of greater than 1%;

[41] the Lp-gRRTC composition of [39], wherein the aqueous pharmaceutically

acceptable carrier is trehalose;

[42] the Lp-gRRTC composition of [41], wherein the pharmaceutically acceptable carrier comprises 1% to 50% trehalose;

[43] the Lp-gRRTC composition according to any of [39] -[42], wherein the

pharmaceutically acceptable carrier comprises 1% to 50% dextrose solution;

[44] the Lp-gRRTC composition according to any of [39] -[43], wherein the interior space of the liposome comprises 5% dextrose suspended in an HEPES buffered solution; [45] the Lp-gRRTC composition according to any of [39] -[44], wherein the pharmaceutically acceptable carrier comprises a buffer such as HEPES Buffered Saline (HBS) or similar, at a concentration of between 1 to 200 mM and a pH of between 2 to 8;

[46] the Lp-gRRTC composition according to any of [39]-[45], wherein the

pharmaceutically acceptable carrier comprises a total concentration of sodium acetate and calcium acetate of between 50 mM to 500 mM;

[47] the Lp-gRRTC composition according to any of [l2]-[46], wherein the interior space of the liposome has a pH of 5-8 or a pH of 6-7, or any range therein between;

[48] the Lp-gRRTC composition according to any of [l2]-[47], wherein the liposome comprises less than 500,000 or less than 200,000 molecules of the gamma polyglutamated pralatrexate;

[49] the Lp-gRRTC composition according to any of [l2]-[48], wherein the liposome comprises between 10 to 100,000 molecules of the gamma polyglutamated pralatrexate, or any range therein between;

[50] the Lp-gRRTC composition according to any of [l2]-[49], which further

comprises a targeting moiety and wherein the targeting moiety has a specific affinity for a surface antigen on a target cell of interest;

[51] the Lp-gRRTC composition according to [50], wherein the targeting moiety is attached to one or both of a PEG and the exterior of the liposome, optionally wherein targeting moiety is attached to one or both of the PEG and the exterior of the liposome by a covalent bond;

[52] the Lp-gRRTC composition of [50] or [51], wherein the targeting moiety is a polypeptide;

[53] the Lp-gRRTC composition according to any of [50] -[52], wherein the targeting moiety is an antibody or an antigen binding fragment of an antibody;

[54] the Lp-gRRTC composition according to any of [50]-[53], wherein the targeting moiety binds the surface antigen with an equilibrium dissociation constant (Kd) in a range of 0.5 x 10 ¹⁰ to 10 x 10 ⁶ as determined using BIACORE®analysis;

[55] the Lp-gRRTC composition according to any of [50]-[54], wherein the targeting moiety specifically binds one or more folate receptors selected from the group consisting of: folate receptor alpha (FR-a), folate receptor beta (FR-b), and folate receptor delta (FR-d);

[56] the Lp-gRRTC composition according to any of [50]-[55], wherein the targeting moiety comprises one or more selected from the group consisting of: an antibody, a humanized antibody, an antigen binding fragment of an antibody, a single chain antibody, a single-domain antibody, a bi-specific antibody, a synthetic antibody, a pegylated antibody, and a multimeric antibody;

[57] the Lp-gRRTC composition according to any of [50]-[56], wherein each

pegylated liposome comprises from 1 to 1000 or 30-200 targeting moieties;

[58] the Lp-gRRTC composition according to any of [39]-[57], further comprising one or more of an immunostimulatory agent, a detectable marker and a maleimide, wherein the immunostimulatory agent, the detectable marker or the maleimide is attached to said PEG or the exterior of the liposome;

[59] the Lp-gRRTC composition of [58], wherein the immunostimulating agent is at least one selected from the group consisting of: a protein immunostimulating agent; a nucleic acid immunostimulating agent; a chemical immunostimulating agent; a hapten; and an adjuvant;

[60] the Lp-gRRTC composition of [58] or [59], wherein the immunostimulating agent is at least one selected from the group consisting of: a fluorescein; a fluorescein isothiocyanate (FITC); a DNP; a beta glucan; a beta-l,3-glucan; a beta-l,6- glucan; a resolvin (e.g., a Resolvin D such as D _n-6DPA or D„ _3DPA, a Resolvin E, or a T series resolvin); and a Toll-like receptor (TLR) modulating agent such as, an oxidized low-density lipoprotein (e.g. OXPAC, PGPC), and an eritoran lipid (e.g., E5564);

[61] the Lp-gRRTC composition according to any of [58] -[60], wherein the

immunostimulatory agent and the detectable marker is the same;

[62] the Lp-gRRTC composition according to any of [58]- [61], further comprising a hapten;

[63] the Lp-gRRTC composition of [62], wherein the hapten comprises one or more of fluorescein or Beta 1, 6-glucan; [64] the Lp-gRRTC composition according to any of [l2]-[63], which further comprises at least one cryoprotectant selected from the group consisting of mannitol; trehalose; sorbitol; and sucrose;

[65] a targeted composition comprising the composition according to any of [l]-[64];

[66] a non-targeted composition comprising the composition according to any of [l]-[49];

[67] the Lp-gRRTC composition according to any of [l2]-[66], which further

comprises carboplatin and/or pembroluzumab;

[68] a pharmaceutical composition comprising the liposomal gamma polyglutamated pralatrexate composition according to any of [l2]-[67];

[69] a pharmaceutical composition comprising gamma polyglutamated pralatrexate composition according to any of [l]-[7];

[70] the composition of any of [l]-[69], for use in the treatment of disease;

[71] use of the composition of any of [l]-[70], in the manufacture of a medicament for the treatment of disease;

[72] a method for treating or preventing disease in a subject needing such treatment or prevention, the method comprising administering the composition of any of [1]- [70] to the subject;

[73] a method for treating or preventing disease in a subject needing such treatment or prevention, the method comprising administering the liposomal gamma polyglutamated pralatrexate composition of any of [12] -[69] to the subject;

[74] a method of killing a hyperproliferative cell that comprises contacting a

hyperproliferative cell with the composition of any of [l]-[69];

[75] a method of killing a hyperproliferative cell that comprises contacting a

hyperproliferative cell with the liposomal gamma polyglutamated pralatrexate composition of any of [l2]-[69];

[76] the method of [74] or [75], wherein the hyperproliferative cell is a cancer cell, a mammalian cell, and/or a human cell;

[77] a method for treating cancer that comprises administering an effective amount of the composition of any of [l]-[69] to a subject having or at risk of having cancer; [78] a method for treating cancer that comprises administering an effective amount of the liposomal gamma polyglutamated pralatrexate composition of any of [12]- [68] to a subject having or at risk of having cancer;

[79] the method of [77] or [78], wherein the cancer is selected from the group

consisting of: a non-hematologic malignancy including such as for example, lung cancer, pancreatic cancer, breast cancer, ovarian cancer, prostate cancer, head and neck cancer, gastric cancer, gastrointestinal cancer, colorectal cancer, esophageal cancer, cervical cancer, liver cancer, kidney cancer, biliary duct cancer, gallbladder cancer, bladder cancer, sarcoma (e.g., osteosarcoma), brain cancer, central nervous system cancer, and melanoma; and a hematologic malignancy such as for example, a leukemia, a lymphoma and other B cell malignancies, myeloma and other plasma cell dyscrasias;

[80] the method of [77] or [78], wherein the cancer is a member selected from the group consisting of: lung cancer, breast cancer, colon cancer, pancreatic cancer, gastric cancer, bladder cancer, head and neck cancer, ovarian cancer, cervical cancer, cancer of the fallopian tubes, and a primary peritoneal cancer;

[81] the method of [77] or [78], wherein the cancer is mesothelioma or non-small cell lung carcinoma (NSCLC);

[82] the method of [77] or [78], wherein the cancer is a lymphoma, such as a T-cell lymphoma (e.g., refractory peripheral T-cell lymphoma (PTCL));

[83] a method for treating cancer that comprises administering an effective amount of the Lp-gRRTC composition of any of [50]-[66] to a subject having or at risk of having a cancer cell that expresses on its surface a folate receptor bound by the targeting moiety;

[84] a maintenance therapy for subjects that are undergoing or have undergone cancer therapy that comprise administering an effective amount of the composition of any of [l]-[69] to a subject that is undergoing or has undergone cancer therapy;

[85] a maintenance therapy for subjects that are undergoing or have undergone cancer therapy that comprise administering an effective amount of the liposomal gamma polyglutamated pralatrexate composition of any of [l2]-[69] to a subject that is undergoing or has undergone cancer therapy; [86] a method for treating a disorder of the immune system that comprises administering an effective amount of the composition of any of [l]-[69] to a subject having or at risk of having a disorder of the immune system;

[87] a method for treating a disorder of the immune system that comprises

administering an effective amount of the liposomal gamma polyglutamated pralatrexate composition of any of [8]-[69] to a subject having or at risk of having a disorder of the immune system;

[88] a method for treating an infectious disease that comprises administering an

effective amount of the composition of any of [l]-[69] to a subject having or at risk of having an infectious disease;

[89] a method for treating an infectious disease that comprises administering an

effective amount of the liposomal gamma polyglutamated pralatrexate composition of any of [l2]-[69] to a subject having or at risk of having an infectious disease;

[90] a method of delivering gamma polyglutamated pralatrexate to a tumor expressing a folate receptor on its surface, the method comprising: administering the Lp- gRRTC composition of any of [l]-[69] to a subject having the tumor in an amount to deliver a therapeutically effective dose of the gamma polyglutamated pralatrexate to the tumor;

[91] a method of preparing a gamma polyglutamated pralatrexate composition

comprising the liposomal gamma polyglutamated pralatrexate composition of any of [l2]-[69], the method comprising: forming a mixture comprising:

liposomal components and gamma polyglutamated antifolate in solution;

homogenizing the mixture to form liposomes in the solution; and processing the mixture to form liposomes containing gamma polyglutamated pralatrexate;

[92] a method of preparing the composition of any of [12] -[69] comprising the steps of: forming a mixture comprising: liposomal components and gamma polyglutamated pralatrexate in a solution; homogenizing the mixture to form liposomes in the solution; processing the mixture to form liposomes entrapping and/or encapsulating gamma polyglutamated pralatrexate; and providing a targeting moiety on a surface of the liposomes, the targeting moiety having specific affinity for at least one of folate receptor alpha (FR-a), folate receptor beta (FR-b) and folate receptor delta (FR-d);

[93] the method according to [92], wherein the processing step includes one or more steps of: thin film hydration, extrusion, in-line mixing, ethanol injection technique, freezing-and-thawing technique, reverse-phase evaporation, dynamic high pressure microfluidization, microfluidic mixing, double emulsion, freeze- dried double emulsion, 3D printing, membrane contactor method, and stirring; and/or

[94] the method according to [92], wherein said processing step includes one or more steps of modifying the size of the liposomes by one or more of steps of extrusion, high-pressure microfluidization, and/or sonication.

[0013] In some embodiments, the disclosure provides a gamma polyglutamated pralatrexate (gRRTC) composition wherein at least 2 of the glutamyl residues of the gamma polyglutamated pralatrexate have a gamma carboxyl group linkage. In some embodiments, the gRRTC contains 2-20, 2-15, 2-10, 2-5, or more than 5, glutamyl groups (including the glutamyl group in pralatrexate). In some embodiments, the gRRTC comprises two or more glutamyl groups in the L-form. In other embodiments, the gRRTC comprises a glutamyl group in the D-form. In further embodiments, the gRRTC comprises a glutamyl group in the D-form and two or more glutamyl groups in the L-form.

[0014] In one embodiment, the gRRTC composition contains a chain of 3 glutamyl groups attached to the glutamyl group of pralatrexate (/. _<?., a tetraglutamated pralatrexate). In some embodiments, the tetraglutamated PTX comprises two or more glutamyl groups in the L- form. In other embodiments, the tetraglutamated PTX comprises a glutamyl group in the D-form. In further embodiments, the tetraglutamated PTX comprises a glutamyl group in the D-form and two or more glutamyl groups in the L-form.

[0015] In one embodiment, the gRRTC composition contains a chain of 4 g-glutamyl groups attached to the glutamyl group of pralatrexate (e.g., g-pentaglutamated pralatrexate). In some embodiments, the gamma pentaglutamated PTX comprises two or more glutamyl groups in the L-form. In other embodiments, the gamma pentaglutamated PTX comprises a glutamyl group in the D-form. In further embodiments, the gamma pentaglutamated PTX comprises a glutamyl group in the D-form and two or more glutamyl groups in the L-form. [0016] In one embodiment, the gRRTC composition contains a chain of 5 g-glutamyl groups attached to the glutamyl group of pralatrexate (e.g., g-hexaglutamated pralatrexate). In some embodiments, the gamma hexaglutamated PTX comprises two or more glutamyl groups in the L-form. In other embodiments, the gamma hexaglutamated PTX comprises a glutamyl group in the D-form. In further embodiments, the gamma hexaglutamated PTX comprises a glutamyl group in the D-form and two or more glutamyl groups in the L-form.

[0017] In additional embodiments, the disclosure provides compositions containing delivery vehicles such as liposomes filled with (e.g., encapsulating) and/or otherwise associated with gamma polyglutamated pralatrexate, and methods of making and using the gRRTC filled/associated delivery vehicle compositions (DV-gRRTC) to deliver gamma polyglutamated pralatrexate to diseased (e.g., cancerous) and/or targeted cells. These compositions have uses that include but are not limited to treating diseases that include for example, hyperproliferative diseases such as cancer, disorders of the immune system such as inflammation and rheumatoid arthritis, and infectious disease such as HIV and malaria. In some embodiments, gamma polyglutamated pralatrexate in the DV-gRRTC contains 2- 20, 2-15, 2-10, 2-5, more than 5, or more than 20, glutamyl groups (including the glutamyl group in pralatrexate). The DV-gRRTC filled/associated delivery vehicle compositions provide improvements to the efficacy and safety of delivering pralatrexate to cancer cells by providing the preferential delivery of a more cytotoxic payload (e.g., polyglutamated pralatrexate) compared to the cytotoxicity of pralatrexate administered in its monoglutamate state (PTX). In some embodiments, a gamma polyglutamated pralatrexate composition provided herein is more cytotoxic to hyperproliferative cells than pralatrexate. In some embodiments the hyperproliferative cells are cancer cells. In some embodiments, the hyperproliferative cells a colorectal carcinoma cells, colon cancer cells, breast cancer cells, or ovarian cancer cells. In some embodiments, the cancer cells are mesothelioma cells or non-small cell lung carcinoma cells. In some embodiments, cytotoxicity is measured in an in vitro assay. In some embodiments, the gamma polyglutamated pralatrexate is a hexaglutamated pralatrexate.

[0018] In some embodiments, a gamma polyglutamated pralatrexate composition provided herein has lower toxic side effects than pralatrexate. In some embodiments, the gamma polyglutamated pralatrexate composition provided herein is less toxic to non- hyperproliferative cells than pralatrexate. In some embodiments, the gamma polyglutamated pralatrexate composition provided herein is less toxic to neutrophils, liver cells, or to colon epithelium cells than pralatrexate. In some embodiments, the neutrophils human neutrophils, differentiating human neutrophils, or neutrophils differentiated from CD34+ cells. In some embodiments, the liver cells are AML12 liver cells. In some embodiments, the colon epithelium cells are CCD841 colon epithelium cells. In some embodiments, the toxicity is measured in an in vitro assay. In some embodiments, the gamma polyglutamated pralatrexate is a hexaglutamated pralatrexate.

[0019] In some embodiments, a gamma polyglutamated pralatrexate composition provided herein has lower toxic side effects than to pralatrexate. In some embodiments, a gamma polyglutamated pralatrexate composition provided herein causes fewer or less severe toxic side effects in an vivo assay than pralatrexate. In some embodiments, the in vivo assay is an in vivo murine model. In some embodiments, a gamma polyglutamated pralatrexate composition provided herein causes fewer or less severe hematological or hepatic toxic side effects than pralatrexate. In some embodiments, hematological side effects are assessed by measuring mean neutrophil, mean white blood cell or mean platelet counts. In some embodiments, hepatic toxic side effects are assessed by measuring serum aspartate transaminase (AST), serum alanine transaminase (ALT), and/or serum albumin levels. In some embodiments, the in vivo assay comprises administering 40 mg/kg or 80 mg/kg of the gamma polyglutamated pralatrexate composition once weekly for 4 weeks. In some embodiments, the gamma polyglutamated pralatrexate is a hexaglutamated pralatrexate.

[0020] In some embodiments, treatment with a gamma polyglutamated pralatrexate composition provided herein does not induce significant hematological or hepatic toxic side effects in an in vivo murine model. In some embodiments, hematological side effects are assessed by measuring mean neutrophil, mean white blood cell or mean platelet counts. In some embodiments, hepatic toxic side effects are assessed by measuring serum aspartate transaminase (AST), serum alanine transaminase (ALT), and/or serum albumin levels. In some embodiments, a gamma polyglutamated pralatrexate composition provided herein does not significantly decrease mean neutrophil, mean white blood cell or mean platelet counts. In some embodiments, a gamma polyglutamated pralatrexate composition provided herein does not significantly increase serum aspartate transaminase (AST) and serum alanine transaminase (ALT) levels. In some embodiments, a gamma polyglutamated pralatrexate composition provided herein does not significantly decrease serum albumin levels. In some embodiments, the in vivo assay comprises administering 40 mg/kg or 80 mg/kg of the gamma polyglutamated pralatrexate composition once weekly for 4 weeks. In some embodiments, the gamma polyglutamated pralatrexate is a hexaglutamated pralatrexate.

[0021] In additional embodiments, the disclosure provides a composition comprising a liposome encapsulating (filled with) gamma polyglutamated pralatrexate (Lp-gRRTC). In some embodiments, the gamma polyglutamated pralatrexate in the Lp-gRRTC contains 2-20, 2-15, 2-10, 2-5, or more than 20, glutamyl groups (including the glutamyl group in pralatrexate). In some embodiments, the gamma polyglutamated pralatrexate in the Lp- gRRTC comprises two or more glutamyl groups in the L-form. In other embodiments, the gamma polyglutamated pralatrexate in the Lp-gRRTC comprises a glutamyl group in the D-form. In further embodiments, the gamma polyglutamated pralatrexate in the Lp-gRRTC comprises a glutamyl group in the D-form and two or more glutamyl groups in the L-form.

[0022] In one embodiment, the Lp-gRRTC composition comprises a gamma polyglutamated PTX that contains a chain of 3 glutamyl groups attached to the glutamyl group of pralatrexate (/. _<?., tetraglutamated pralatrexate). In some embodiments, the tetraglutamated PTX comprises two or more glutamyl groups in the L-form. In other embodiments, the tetraglutamated PTX comprises a glutamyl group in the D-form. In further embodiments, the tetraglutamated PTX comprises a glutamyl group in the D-form and two or more glutamyl groups in the L-form.

[0023] In one embodiment, the Lp-gRRTC composition comprises a gamma polyglutamated PTX that contains a chain of 4 g-glutamyl groups attached to the glutamyl group of pralatrexate (e.g., g-pentaglutamated pralatrexate). In some embodiments, the gamma pentaglutamated PTX comprises two or more glutamyl groups in the L-form. In other embodiments, the gamma pentaglutamated PTX comprises a glutamyl group in the D-form. In further embodiments, the gamma pentaglutamated PTX comprises a glutamyl group in the D-form and two or more glutamyl groups in the L-form.

[0024] In one embodiment, the Lp-gRRTC composition comprises a gamma polyglutamated PTX that contains a chain of 5 g-glutamyl groups attached to the glutamyl group of pralatrexate (e.g., g-hexaglutamated pralatrexate). In some embodiments, the gamma hexaglutamated PTX comprises two or more glutamyl groups in the L-form. In other embodiments, the gamma hexaglutamated PTX comprises a glutamyl group in the D- form. In further embodiments, the gamma hexaglutamated PTX comprises a glutamyl group in the D-form and two or more glutamyl groups in the L-form.

[0025] In some embodiments, the Lp-gRRTC composition is cationic. In some embodiments, the Lp-gRRTC liposome is cationic and has a diameter in the range of 20 nm to 500 nm, 20 nm to 200 nm, 30 nm to 175 nm, or 50 nm to 150 nm, or any range therein between. In further embodiments, the Lp-gRRTC liposome is cationic and the composition has a diameter in the range of 80 nm to 120 nm, or any range therein between. In some embodiments, the cationic Lp-gRRTC composition comprises at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, w/w of the gamma polyglutamated PTX. In some embodiments, during the process of preparing the Lp-gRRTC, at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, of the starting material of gamma polyglutamated PTX is encapsulated (entrapped) in the cationic Lp-gRRTC. In additional embodiments, the gamma polyglutamated pralatrexate encapsulated by the liposome is in a HEPES buffered solution within the liposome.

[0026] In other embodiments, Lp-gRRTC composition is anionic or neutral. In some embodiments, the Lp-gRRTC liposome is anionic or neutral and has a diameter in the range of 20 nm to 500 nm, 20 nm to 200 nm, 30 nm to 175 nm, or 50 nm to 150 nm, or any range therein between. In further embodiments, the Lp-gRRTC liposome is anionic or neutral and the composition has a diameter in the range of 80 nm to 120 nm, or any range therein between. In some embodiments, the Lp-gRRTC liposome is anionic and has a diameter in the range of 20 nm to 500 nm, 20 nm to 200 nm, 30 nm to 175 nm, or 50 nm to 150 nm, or any range therein between. In further embodiments, the Lp-gRRTC liposome is anionic and the composition has a diameter in the range of 80 nm to 120 nm, or any range therein between. In some embodiments, the Lp-gRRTC liposome is neutral and has a diameter in the range of 20 nm to 500 nm, 20 nm to 200 nm, 30 nm to 175 nm, or 50 nm to 150 nm, or any range therein between. In some embodiments, the anionic or neutral Lp-gRRTC composition comprises at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, w/w of the gamma polyglutamated PTX. In some embodiments, during the process of preparing the Lp-gRRTC, at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, of the starting material of gamma polyglutamated PTX is encapsulated (entrapped) in the anionic or neutral Lp-gRRTC. In some embodiments, the anionic or neutral Lp-gRRTC composition comprises at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, w/w of the gamma tetraglutamated PTX. In some embodiments, the anionic or neutral Lp-gRRTC composition comprises at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, w/w of the gamma pentaglutamated PTX. In some embodiments, the anionic or neutral Lp-gRRTC composition comprises at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, w/w of the gamma hexaglutamated PTX. In additional embodiments, the gamma polyglutamated pralatrexate encapsulated by the liposome is in a HEPES buffered solution within the liposome.

[0027] In additional embodiments, the liposomal gamma polyglutamated pralatrexate composition is pegylated (PLp-gRRTC).

[0028] In some embodiments, the liposomal gamma polyglutamated pralatrexate composition is non-targeted (NTLp-gRRTC). That is, the NTLp-gRRTC composition does not have specific affinity towards an epitope (e.g., an epitope on a surface antigen) expressed on the surface of a target cell of interest. In further embodiments, the non- targeted liposomal gamma polyglutamated pralatrexate composition is pegylated (NTPLp- gRRTC).

[0029] In other embodiments, the liposomal gamma polyglutamated pralatrexate composition is targeted (TLp-gRRTC). That is, the TLp-gRRTC composition contains a targeting moiety that has specific affinity for an epitope (surface antigen) on a target cell of interest. In some embodiments, the targeting moiety of the TLp-gRRTC or TPLp-gRRTC is not attached to the liposome through a covalent bond. In other embodiments, the targeting moiety of the TLp-gRRTC or TPLp-gRRTC is attached to one or both of a PEG and the exterior of the liposome. Targeted liposomal gamma polyglutamated pralatrexate compositions (TLp-gRRTC and TPLp-gRRTC) provide further improvements over the efficacy and safety profile of pralatrexate, by specifically delivering gamma polyglutamated (e.g., g-pentaglutamated and/or g-hexaglutamated) pralatrexate to target cells such as cancer cells. In some embodiments, the targeted liposomal gamma polyglutamated pralatrexate composition is pegylated (TPLp-gRRTC). In some embodiments, the targeting moiety of the TLp-gRRTC or TPLp-gRRTC is attached to one or both of a PEG and the exterior of the liposome. In some embodiments, the targeting moiety of the TLp-gRRTC or TPLp-gRRTC is attached to the liposome through a covalent bond. Function of the targeting moiety of the TLp-gRRTC and/or TPLp-gRRTC compositions include but are not limited to, targeting the liposome to the target cell of interest in vivo or in vitro; interacting with the surface antigen for which the targeting moiety has specific affinity, and delivering the liposome payload (gRRTC) into the cell. Suitable targeting moieties are known in the art and include, but are not limited to, antibodies, antigen-binding antibody fragments, scaffold proteins, polypeptides, and peptides. In some embodiments, the targeting moiety is a polypeptide. In further embodiments, the targeting moiety is a polypeptide that comprises at least 3, 5, 10, 15, 20, 30, 40, 50, or 100, amino acid residues.

[0030] In some embodiments, the targeting moiety of the TLp-gRRTC or TPLp-gRRTC is an antibody or an antigen-binding antibody fragment. In further embodiments, the targeting moiety comprises one or more of an antibody, a humanized antibody, an antigen binding fragment of an antibody, a single chain antibody, a single-domain antibody, a bi-specific antibody, a synthetic antibody, a pegylated antibody, and a multimeric antibody. In some embodiments, the targeting moiety of the TLp-gRRTC or TPLp-gRRTC has specific affinity for an epitope that is preferentially expressed on a target cell such as a tumor cell, compared to normal or non-tumor cells. In some embodiments, the targeting moiety has specific affinity for an epitope on a tumor cell surface antigen that is present on a tumor cell but absent or inaccessible on a non-tumor cell. In some embodiments, the targeting moiety binds an epitope of interest with an equilibrium dissociation constant (Kd) in a range of 0.5 x 10 ¹⁰ to 10 x 10 ⁶ as determined using BIACORE® analysis.

[0031] In particular embodiments, the TLp-gRRTC or TPLp-gRRTC targeting moiety comprises a polypeptide that specifically binds a folate receptor. In some embodiments, the targeting moiety is an antibody or an antigen-binding antibody fragment. In some embodiments, the folate receptor bound by the targeting moiety is one or more folate receptors selected from the group consisting of: folate receptor alpha (FR-a, FOLR1), folate receptor beta (FR-b, FOLR2), and folate receptor delta (FR-d, FOLR4). In some embodiments, the folate receptor bound by the targeting moiety is folate receptor alpha (FR-a). In some embodiments, the folate receptor bound by the targeting moiety is folate receptor beta (FR-b). In some embodiments, the targeting moiety specifically binds FR-a and FR-b.

[0032] In additional embodiments, the Lp-gRRTC composition comprises one or more of an immunostimulatory agent, a detectable marker, and a maleimide, disposed on at least one of the PEG and the exterior of the liposome. In some embodiments, the liposome gRRTC composition (e.g., Lp-gRRTC, PLp-gRRTC, NTLp-gRRTC, NTPLp-gRRTC, TLp- gRRTC, or TPLp-gRRTC) is cationic. In other embodiments, the liposome gRRTC composition (e.g., Lp-gRRTC, PLp-gRRTC, NTLp-gRRTC, NTPLp-gRRTC, TLp-gRRTC or TPLp-gRRTC) is anionic or neutral. In additional embodiments, the liposome of the liposome gRRTC composition (e.g., Lp-gRRTC, PLp-gRRTC, NTLp-gRRTC, NTPLp- gRRTC, TLp-gRRTC or TPLp-gRRTC) has a diameter in the range of 20 nm to 500 nm, 20 nm to 200 nm, 30 nm to 175 nm, 50 nm to 150 nm, or any range therein between. In some embodiments, the liposome of the liposome-gRRTC composition has a diameter in the range of 30 nm to 175 nm or 50 nm to 150 nm, or any range therein between. In further embodiments, the liposome of the liposome gRRTC composition has a diameter in the range of 80 nm to 120 nm, or any range therein between. In some embodiments, the liposome gRRTC composition is pegylated (e.g., PLp-gRRTC, NTPLp-gRRTC, or TPLp-gRRTC). In some embodiments, the liposome gRRTC composition comprises a targeting moiety (e.g., TLp-gRRTC or TPLp-gRRTC). In further embodiments, the liposome gRRTC composition is pegylated and targeted (e.g., TPLp-gRRTC). In some embodiments, the liposome gRRTC composition comprises gamma poly glutamated pralatrexate that contains 4, 5, 2-10, 4-6, or more than 5, glutamyl groups. In some embodiments, the liposome gRRTC composition comprises gamma tetraglutamated pralatrexate. In some embodiments, the liposome gRRTC composition comprises gamma pentaglutamated pralatrexate. In other embodiments, the liposome gRRTC composition comprises gamma hexaglutamated pralatrexate.

[0033] In some embodiments, the liposome compositions comprise of gamma polyglutamated pralatrexate that contains 4, 5, 2-10, 4-6, or more than 5, glutamyl groups and at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, w/w of the gamma polyglutamated PTX. In some embodiments, the Lp-gRRTC composition comprises gamma polyglutamated pralatrexate that contains 4, 5, 2-10, 4-6, or more than 5, glutamyl groups and l%-98.5% w/w of the gamma polyglutamated PTX. In some embodiments, the liposomes comprise gamma polyglutamated pralatrexate that contains 4, 5, 2-10, 4-6, or more than 5, glutamyl groups and wherein during the process of preparing the Lp-gRRTC, at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75% of the starting material of gamma polyglutamated PTX is encapsulated (entrapped) in the Lp- gRRTC.

[0034] In some embodiments, the liposome compositions comprise of gamma tetraglutamated pralatrexate and at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, w/w of the gamma tetraglutamated PTX. In some embodiments, the Lp-gRRTC composition comprises gamma tetraglutamated pralatrexate and l%-98.5% w/w of the gamma tetraglutamated PTX. In some embodiments, the liposomes comprise gamma tetraglutamated pralatrexate and wherein during the process of preparing the Lp-gRRTC, at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75% of the starting material of gamma tetraglutamated PTX is encapsulated (entrapped) in the Lp- gRRTC.

[0035] In some embodiments, the liposome compositions comprise of gamma pentaglutamated pralatrexate and at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, w/w of the gamma pentaglutamated PTX. In some embodiments, the Lp-gRRTC composition comprises gamma pentaglutamated pralatrexate and l%-98.5% w/w of the gamma pentaglutamated PTX. In some embodiments, the liposomes comprise gamma pentaglutamated pralatrexate and wherein during the process of preparing the Lp-gRRTC, at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75% of the starting material of gamma pentaglutamated PTX is encapsulated (entrapped) in the Lp- gRRTC. In some embodiments, the liposome compositions comprise of gamma hexaglutamated pralatrexate and at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75%, w/w of the gamma hexaglutamated PTX. In some embodiments, the Lp-gRRTC composition comprises gamma hexaglutamated pralatrexate and l%-98.5% w/w of the gamma hexaglutamated PTX. In some embodiments, the liposomes comprise gamma hexaglutamated pralatrexate and wherein during the process of preparing the Lp-gRRTC, at least 1%, 5%, 10%, 15%, 20%, 25%, 30%, 35%, 40%, 45%, 50%, 55%, 60%, 65%, 70%, 75%, or more than 75% of the starting material of gamma pentaglutamated PTX is encapsulated (entrapped) in the Lp- gRRTC.

[0036] Liposomal compositions comprising liposomes encapsulating gRRTC are also provided. In some embodiments, the liposomal composition comprises a pegylated gRRTC composition. In some embodiments, the liposomal composition comprises a gRRTC composition that is linked to or otherwise associated with a targeting moiety. In further embodiments, the liposomal composition comprises a gRRTC composition that is pegylated and linked to or otherwise associated with a targeting moiety. In some embodiments, the liposomal composition comprises gRRTC that contains 4, 5, 2-10, 4-6, or more than 5, glutamyl groups. In some embodiments, the liposomal composition comprises gamma tetraglutamated pralatrexate. In some embodiments, the liposomal composition comprises gamma pentaglutamated pralatrexate. In other embodiments, the liposomal composition comprises gamma hexaglutamated pralatrexate.

[0037] In some embodiments, the liposomal composition comprises a liposome gRRTC

(e.g., Lp-gRRTC, PLp-gRRTC, NTLp-gRRTC, NTPLp-yPPTX, TLp-gRRTC, and TPLp- gRRTC). In some embodiments, the liposome gRRTC is pegylated (e.g., NTPLp-yPPTX, and TPLp-gRRTC). In some embodiments, the liposome gRRTC comprises a targeting moiety that has a specific affinity for an epitope of antigen on the surface of a target cell of interest such as a cancer cell (e.g., TLp-gRRTC or TPLp-gRRTC)). In further embodiments, the liposomal composition comprises a liposome gRRTC that is pegylated and further comprises a targeting moiety that has a specific affinity for an epitope of antigen on the surface of a target cell of interest such as a cancer cell (e.g., TPLp-gRRTC). In some embodiments, the liposomal composition comprises a liposome gRRTC that is cationic. In other embodiments, the liposomal composition comprises a liposome gRRTC that is anionic or neutral. In additional embodiments, the liposomal composition comprises a liposome gRRTC that has a diameter in the range of 20 nm to 500 nm, 20 nm to 200 nm, or any range therein between. In further embodiments, the liposome gRRTC has a diameter in the range of 80 nm to 120 nm, or any range therein between.

[0038] Pharmaceutical compositions comprising gamma polyglutamated pralatrexate

(gRRTC) including delivery vehicles such as liposome gRRTC are also provided. In some embodiments, the pharmaceutical composition comprises a pegylated gRRTC composition. In some embodiments, the pharmaceutical composition comprise a gRRTC composition that is linked to or otherwise associated with a targeting moiety. In further embodiments, the pharmaceutical composition comprise a gRRTC composition that is pegylated and linked to or otherwise associated with a targeting moiety. In some embodiments, the pharmaceutical composition comprises gRRTC that contains 4, 5, 2-10, 4-6, or more than 5, glutamyl groups. In some embodiments, the pharmaceutical composition comprises gamma tetraglutamated pralatrexate. In some embodiments, the pharmaceutical composition comprises gamma pentaglutamated pralatrexate. In other embodiments, the pharmaceutical composition comprises gamma hexaglutamated pralatrexate.

[0039] In some embodiments, the pharmaceutical compositions comprise a liposome gRRTC (e.g., Lp-gRRTC, PLp-gRRTC, NTLp-gRRTC, NTPLp-yPPTX, TLp-gRRTC, and TPLp-gRRTC). In some embodiments, the liposome gRRTC composition is pegylated (e.g., NTPLp-gRRTC, and TPLp-gRRTC). In some embodiments, the liposome gRRTC comprises a targeting moiety that has a specific affinity for an epitope of antigen on the surface of a target cell of interest such as a cancer cell (e.g., TLp-gRRTC or TPLp-gRRTC)). In further embodiments, the pharmaceutical composition comprises a liposome gRRTC composition that is pegylated and further comprises a targeting moiety that has a specific affinity for an epitope of antigen on the surface of a target cell of interest such as a cancer cell (e.g., TPLp-gRRTC). In some embodiments, the pharmaceutical composition comprises a liposome gRRTC that is cationic. In other embodiments, the pharmaceutical composition comprises a liposome gRRTC that is anionic or neutral. In additional embodiments, the pharmaceutical composition comprises a liposome gRRTC that has a diameter in the range of 20 nm to 500 nm or 20 nm to 500 nm, or any range therein between. In further embodiments, the liposome gRRTC composition has a diameter in the range of 80 nm to 120 nm, or any range therein between.

[0040] In additional embodiments, the disclosure provides a method of killing a cell that comprises contacting the cell with a composition comprising a gamma polyglutamated pralatrexate (gRRTC) composition (e.g., a gRRTC disclosed herein). In some embodiments, the contacted cell is a mammalian cell. In further embodiments, the contacted cell is a human cell. In some embodiments, the contacted cell is a hyperproliferative cell. In further embodiments, the hyperproliferative cell is a cancer cell. In further embodiments, the contacted cancer cell is a primary cell or a cell from a cell line obtained/derived from a cancer selected from the group consisting of: a non-hematologic malignancy including such as for example, lung cancer, pancreatic cancer, breast cancer, ovarian cancer, prostate cancer, head and neck cancer, gastric cancer, gastrointestinal cancer, colorectal cancer, esophageal cancer, cervical cancer, liver cancer, kidney cancer, biliary duct cancer, gallbladder cancer, bladder cancer, sarcoma (e.g., osteosarcoma), brain cancer, central nervous system cancer, and melanoma; and a hematologic malignancy such as for example, a leukemia, a lymphoma and other B cell malignancies, myeloma and other plasma cell dysplasias or dyscrasias. In some embodiments, the method is performed in vivo. In other embodiments, the method is performed in vitro. In some embodiments, the gRRTC contains 4, 5, 2-10, 4-6, or more than 5, g-glutamyl groups. In some embodiments the gRRTC comprises g-glutamyl groups in the D-form. In some embodiments, the gRRTC contains 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the D-form. In some embodiments the gRRTC comprises g-glutamyl groups in the L-form. In some embodiments, the gRRTC contains 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the L-form. In some embodiments the gRRTC comprises g-glutamyl groups in the L and D-form. In some embodiments the gRRTC contains 2, 3, 4, 5, or more than 5, g- glutamyl groups in the L-form, and 1, 2, 3, 4, 5 or more than 5, g-glutamyl groups in the D-form. In some embodiments, the gRRTC composition comprises gamma tetraglutamated pralatrexate. In some embodiments, the gRRTC composition comprises gamma pentaglutamated pralatrexate. In other embodiments, the gRRTC composition comprises gamma hexaglutamated pralatrexate.

[0041] In additional embodiments, the disclosure provides a method of killing a cell that comprises contacting the cell with a liposome containing gamma polyglutamated pralatrexate (e.g., an Lp-gRRTC such as, PLp-gRRTC, NTLp-gRRTC, NTPLp-gRRTC, TLp-gRRTC or TPLp-gRRTC). In some embodiments, the contacted cell is a mammalian cell. In further embodiments, the contacted cell is a human cell. In some embodiments, the contacted cell is a hyperproliferative cell. In yet further embodiments, the contacted hyperproliferative cell is a cancer cell. In further embodiments, the cancer cell is a primary cell or a cell from a cell line obtained/derived from a cancer selected from the group consisting of: a non-hematologic malignancy including such as for example, lung cancer, pancreatic cancer, breast cancer, ovarian cancer, prostate cancer, head and neck cancer, gastric cancer, gastrointestinal cancer, colorectal cancer, esophageal cancer, cervical cancer, liver cancer, kidney cancer, biliary duct cancer, gallbladder cancer, bladder cancer, sarcoma (e.g., osteosarcoma), brain cancer, central nervous system cancer, and melanoma; and a hematologic malignancy such as for example, a leukemia, a lymphoma and other B cell malignancies, myeloma and other plasma cell dysplasias or dyscrasias. In some embodiments, the method is performed in vivo. In other embodiments, the method is performed in vitro. In some embodiments, the liposome contains a gRRTC containing 4, 5, 2-10, 4-6, or more than 5, glutamyl groups. In some embodiments, the liposome contains gamma tetraglutamated pralatrexate. In some embodiments, the liposome contains gamma pentaglutamated pralatrexate. In other embodiments, the liposome contains gamma hexaglutamated pralatrexate.

[0042] In some embodiments, the liposome comprises a gRRTC containing 4, 5, 2-10, 4- 6, or more than 5, g-glutamyl groups. In some embodiments, the liposome comprises a gRRTC comprising a g-glutamyl group in the D-form. In some embodiments, the liposome comprises a gRRTC containing 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the D-form. In some embodiments, the liposome comprises a gRRTC comprising g-glutamyl groups in the L-form. In some embodiments, the liposome comprises a gRRTC containing 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the L-form. In some embodiments, the liposome comprises a gRRTC comprising g-glutamyl groups in the L form and the D form. In some embodiments the liposome comprises an gRRTC containing 2, 3, 4, 5, or more than 5, g-glutamyl groups in the L-form, and 1, 2, 3, 4, 5 or more than 5, g-glutamyl groups in the D-form. In some embodiments, the liposome comprises gamma pentaglutamated pralatrexate. In other embodiments, the liposome comprises gamma hexaglutamated pralatrexate.

[0043] In additional embodiments, the disclosure provides a method for treating cancer that comprises administering an effective amount of a delivery vehicle ((e.g., an immunoconjugate or liposome) comprising gamma polyglutamated pralatrexate to a subject having or at risk of having cancer. In some embodiments, the delivery vehicle is an antibody-containing immunoconjugate (comprising e.g., a full-length IgG antibody, a bispecific antibody, or a scFv). In some embodiments, the delivery vehicle is a liposome (e.g., an Lp-gRRTC such as, PLp-gRRTC, NTLp-gRRTC, NTPLp-yPPTX, TLp-gRRTC, or TPLp-gRRTC). In some embodiments, the administered delivery vehicle is pegylated. In some embodiments, the administered delivery vehicle is not pegylated. In additional embodiments, the administered delivery vehicle comprises a targeting moiety that has a specific affinity for an epitope of antigen on the surface of a cancer cell. In additional embodiments, the delivery vehicle comprises a targeting moiety that has specific affinity for an epitope of a cell surface antigen selected from the group consisting of: GONMB, TACSTD2 (TROP2), CEACAM5, EPCAM, a folate receptor (e.g., folate receptor-a, folate receptor-b or folate receptor-d), Mucin 1 (MUC-l), MUC-6, STEAP1, mesothelin, Nectin 4, ENPP3, Guanylyl cyclase C (GCC), SLC44A4, NaPi2b, CD70 (TNFSF7), CA9 (Carbonic anhydrase), 5T4 (TPBG), SLTRK6, SC-16, Tissue factor, LIV-l (ZIP6), CGEN- 15027, P Cadherin, Fibronectin Extra-domain B (ED-B), VEGFR2 (CD309), Tenascin, Collagen IV, Periostin, endothelin receptor, HER2, HER3, ErbB4, EGFR, EGFRvIII, FGFR1, FGFR2, FGFR3, FGFR4, FGFR6, IGFR-l, FZD1, FZD2, FZD3, FZD4, FZD5, FZD6, FZD7, FZD8, FZD9, FZD10, SMO, CD2, CD3, CD4, CD5, CD6, CD8, CD11, CDl la, CD15, CD18, CD19, CD20, CD22, CD26, CD27L, CD28, CD30, CD33, CD34, CD37, CD38, CD40, CD44, CD56, CD70, CD74, CD79, CD79b, CD98, CD105, CD133, CD138, cripto, IGF-1R, IGF-2R, EphAl an EphA receptor, an EphB receptor, EphAl, EphA2, EphA3, EphA4, EphA5, EphA6, EphA7, EphA8, EphBl, EphB2, EphB3, EphB4, EphB6, an integrin (e.g., integrin anb3, anb5, or anbό), a C242 antigen, Apo2, PSGR, NGEP, PSCA, TMEFF2, endoglin, PSMA, CanAg, CALLA, c-Met, VEGFR-l, VEGFR- 2, DDR1, PDGFR alpha., PDGFR beta, TrkA, TrkB, TrkC, UFO, LTK, ALK, Tiel, Tie2, PTK7, Ryk, TCR, NMDAR, LNGFR, and MuSK. In some embodiments, the delivery vehicle comprises a targeting moiety that specifically binds a cell surface antigen(s) derived from, or determined to be expressed on, a specific subject’s cancer (tumor) such as a neoantigen. In some embodiments, the targeting moiety has specific affinity for an epitope of a cell surface antigen(s) derived from or determined to be expressed on a specific subject’s tumor such as a neoantigen. In some embodiments, the targeting moiety is an antibody or an antigen binding antibody fragment. In some embodiments, the administered delivery vehicle comprises gRRTC containing 4, 5, 2-10, 4-6, or more than 5, g-glutamyl groups. In some embodiments, the delivery vehicle comprises a gRRTC containing 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the D-form. In some embodiments, the delivery vehicle comprises a gRRTC containing 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the L-form. In some embodiments the delivery vehicle comprises an gRRTC containing 2, 3, 4, 5, or more than 5, g-glutamyl groups in the L-form, and 1, 2, 3, 4, 5 or more than 5, g-glutamyl groups in the D-form. In some embodiments, the administered delivery vehicle comprises gamma tetraglutamated pralatrexate. In some embodiments, the administered delivery vehicle comprises gamma pentaglutamated pralatrexate. In other embodiments, the administered delivery vehicle comprises gamma hexaglutamated pralatrexate. In some embodiments, the administered delivery vehicle comprises L gamma polyglutamated pralatrexate. In some embodiments, the administered delivery vehicle comprises D gamma polyglutamated pralatrexate. In further embodiments, the administered delivery vehicle comprises L and D gamma polyglutamated pralatrexate. In some embodiments, the cancer is selected from the group consisting of: a non- hematologic malignancy including such as for example, lung cancer, pancreatic cancer, breast cancer, ovarian cancer, prostate cancer, head and neck cancer, gastric cancer, gastrointestinal cancer, colorectal cancer, esophageal cancer, cervical cancer, liver cancer, kidney cancer, biliary duct cancer, gallbladder cancer, bladder cancer, sarcoma, brain cancer, central nervous system cancer, and melanoma; and a hematologic malignancy such as for example, a leukemia, a lymphoma and other B cell malignancies, myeloma and other plasma cell dysplasias or dyscrasias.

[0044] In additional embodiments, the disclosure provides a method for treating cancer that comprises administering an effective amount of a liposome comprising gamma polyglutamated pralatrexate (e.g., an Lp-gRRTC such as, PLp-gRRTC, NTLp-gRRTC, NTPLp-gRRTC, TLp-gRRTC, or TPLp-gRRTC) to a subject having or at risk of having cancer. In some embodiments, the liposome is pegylated. In some embodiments, the liposome is not pegylated. In additional embodiments, the liposome comprises a targeting moiety that has a specific affinity for an epitope of antigen on the surface of a cancer cell. In additional embodiments, the liposome comprises a targeting moiety that has specific affinity for an epitope of a cell surface antigen selected from the group consisting of: GONMB, TACSTD2 (TROP2), CEACAM5, EPCAM, a folate receptor (e.g., folate receptor-a, folate receptor-b or folate receptor-d), Mucin 1 (MUC-l), MUC-6, STEAP1, mesothelin, Nectin 4, ENPP3, Guanylyl cyclase C (GCC), SLC44A4, NaPi2b, CD70 (TNFSF7), CA9 (Carbonic anhydrase), 5T4 (TPBG), SLTRK6, SC-16, Tissue factor, LIV-l (ZIP6), CGEN- 15027, P Cadherin, Fibronectin Extra-domain B (ED-B), VEGFR2 (CD309), Tenascin, Collagen IV, Periostin, endothelin receptor, HER2, HER3, ErbB4, EGER, EGFRvIII, FGFR1, FGFR2, FGFR3, FGFR4, FGFR6, IGFR-l, FZD1, FZD2, FZD3, FZD4, FZD5, FZD6, FZD7, FZD8, FZD9, FZD10, SMO, CD2, CD3, CD4, CD5, CD6, CD8, CD11, CDlla, CD15, CD18, CD19, CD20, CD22, CD26, CD27L, CD28, CD30, CD33, CD34, CD37, CD38, CD40, CD44, CD56, CD70, CD74, CD79, CD79b, CD98, CD105, CD133, CD138, cripto, IGF-1R, IGF-2R, EphAl an EphA receptor, an EphB receptor, EphAl, EphA2, EphA3, EphA4, EphA5, EphA6, EphA7, EphA8, EphBl, EphB2, EphB3, EphB4, EphB6, an integrin (e.g., integrin anb3, anb5, or anbό), a C242 antigen, Apo2, PSGR, NGEP, PSCA, TMEFF2, endoglin, PSMA, CanAg, CALLA, c- Met, VEGFR-l, VEGFR-2, DDR1, PDGFR alpha., PDGFR beta, TrkA, TrkB, TrkC, UFO, LTK, ALK, Tiel, Tie2, PTK7, Ryk, TCR, NMDAR, LNGFR, and MuSK.This also includes the use of cancer stem cell targeting moieties such as those targeting CD 34, CD133 and CD44, CD138, and CD15. In some embodiments, the liposome comprises a targeting moiety that has specific affinity for an epitope of a cell surface antigen(s) derived from or determined to be expressed on a specific subject’s tumor such as a neoantigen. In some embodiments, the targeting moiety is an antibody or an antigen binding antibody fragment. In some embodiments, the liposome comprises gRRTC containing 4, 5, 2-10, 4- 6, or more than 5, glutamyl groups. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing g-glutamyl groups in the L-form. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the L- form. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing g-glutamyl groups in the L and D-forms. In some embodiments, a liposome of the administered liposomal composition comprises an gRRTC containing 2, 3, 4, 5, or more than 5, g-glutamyl groups in the L-form, and 1, 2, 3, 4, 5 or more than 5, g-glutamyl groups in the D-form. In some embodiments the administered liposomal composition comprises tetraglutamated gRRTC. In some embodiments the administered liposomal composition comprises pentaglutamated gRRTC. In some embodiments the administered liposomal composition comprises hexaglutamated gRRTC. In some embodiments, the cancer is selected from the group consisting of: lung (e.g., non small lung cancer), pancreatic cancer, breast cancer, ovarian cancer, prostate cancer, head and neck cancer, gastric cancer, gastrointestinal cancer, colorectal cancer, esophageal cancer, cervical cancer, liver cancer, kidney cancer, biliary duct cancer, gallbladder cancer, bladder cancer, sarcoma (e.g. , osteosarcoma), brain cancer, central nervous system cancer, melanoma, and a hematologic malignancy (e.g., a leukemia or lymphoma).

[0045] In additional embodiments, the disclosure provides a method for treating cancer that comprises administering to a subject having or at risk of having cancer, an effective amount of a liposomal composition comprising a liposome that comprises gamma polyglutamated pralatrexate and a targeting moiety that has a specific affinity for an epitope of antigen on the surface of the cancer. In some embodiments, the liposome comprises a targeting moiety that has specific affinity for an epitope of a cell surface antigen selected from the group consisting of: GONMB, TACSTD2 (TROP2), CEACAM5, EPCAM, a folate receptor (e.g., folate receptor-a, folate receptor-b or folate receptor-d), Mucin 1 (MUC-l), MUC-6, STEAP1, mesothelin, Nectin 4, ENPP3, Guanylyl cyclase C (GCC), SLC44A4, NaPi2b, CD70 (TNFSF7), CA9 (Carbonic anhydrase), 5T4 (TPBG), SLTRK6, SC-16, Tissue factor, LIV-l (ZIP6), CGEN-15027, P Cadherin, Fibronectin Extra-domain B (ED-B), VEGFR2 (CD309), Tenascin, Collagen IV, Periostin, endothelin receptor, HER2, HER3, ErbB4, EGFR, EGFRvIII, FGFR1, FGFR2, FGFR3, FGFR4, FGFR6, IGFR-l, FZD1, FZD2, FZD3, FZD4, FZD5, FZD6, FZD7, FZD8, FZD9, FZD10, SMO, CD2, CD3, CD4, CD5, CD6, CD8, CD11, CDlla, CD15, CD18, CD 19, CD20, CD22, CD26, CD27L, CD28, CD30, CD33, CD34, CD37, CD38, CD40, CD44, CD56, CD70, CD74, CD79, CD79b, CD98, CD105, CD133, CD138, cripto, IGF-1R, IGF-2R, EphAl an EphA receptor, an EphB receptor, EphAl, EphA2, EphA3, EphA4, EphA5, EphA6, EphA7, EphA8, EphBl, EphB2, EphB3, EphB4, EphB6, an integrin (e.g., integrin anb3, anb5, or anbό), a C242 antigen, Apo2, PSGR, NGEP, PSCA, TMEFF2, endoglin, PSMA, CanAg, CALLA, c-Met, VEGFR-l, VEGFR-2, DDR1, PDGFR alpha., PDGFR beta, TrkA, TrkB, TrkC, UFO, LTK, ALK, Tiel, Tie2, PTK7, Ryk, TCR, NMDAR, LNGFR, and MuSK. In some embodiments, the liposome comprises a targeting moiety that a targeting moiety that has specific affinity for an epitope of a cell surface antigen(s) derived from, or determined to be expressed on, a specific subject’s cancer (tumor) such as a neoantigen. In some embodiments, the targeting moiety is an antibody or an antigen binding antibody fragment. In some embodiments, the liposome comprises gRRTC containing 4, 5, 2-10, 4-6, or more than 5, g-glutamyl groups. In some embodiments, the liposome comprises a gRRTC containing g-glutamyl groups in the L-form. In some embodiments, the liposome comprises a gRRTC containing 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the L-form. In some embodiments, the liposome comprises a gRRTC containing g-glutamyl groups in the D-form. In some embodiments, the liposome comprises a gRRTC containing 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the D-form. In some embodiments, the liposome comprises a gamma tetraglutamated pralatrexate. In some embodiments, the liposome comprises a gamma pentaglutamated pralatrexate. In some embodiments, the liposome comprises a gamma hexaglutamated pralatrexate.

[0046] In some embodiments, the administered liposomal composition comprises pegylated liposomes (e.g., TPLp-gRRTC). In some embodiments, the administered liposomal composition comprises liposomes that are not pegylated. In some embodiments, liposomes of the administered liposomal composition comprise a gRRTC containing 4, 5, 2- 10, 4-6, or more than 5, gamma glutamyl groups. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing g-glutamyl groups in the D-form. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the D-form. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing g-glutamyl groups in the L-form. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the L-form. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing g- glutamyl groups in the L and D-forms. In some embodiments, a liposome of the administered liposomal composition comprises an gRRTC containing 2, 3, 4, 5, or more than 5, g-glutamyl groups in the L-form, and 1, 2, 3, 4, 5 or more than 5, g-glutamyl groups in the D-form. In in some embodiments, liposomes of the administered liposomal composition comprise gamma tetraglutamated pralatrexate. In in some embodiments, liposomes of the administered liposomal composition comprise gamma pentaglutamated pralatrexate. In other embodiments, liposomes of the administered liposomal composition comprise gamma hexaglutamated pralatrexate. In some embodiments, the liposomal composition is administered to treat a cancer selected from the group consisting of: lung cancer (e.g., non small cell), pancreatic cancer, breast cancer, ovarian cancer, prostate cancer, head and neck cancer, gastric cancer, gastrointestinal cancer, colorectal cancer, esophageal cancer, cervical cancer, liver cancer, kidney cancer, biliary duct cancer, gallbladder cancer, bladder cancer, sarcoma (e.g., osteosarcoma), brain cancer, central nervous system cancer, melanoma, myeloma, a leukemia and a lymphoma.

[0047] In additional embodiments, the disclosure provides a method for treating cancer that comprises administering an effective amount of a liposomal composition to a subject having or at risk of having a cancer that expresses folate receptor on its cell surface, wherein the liposomal composition comprises liposomes that comprise (a) gamma polyglutamated pralatrexate (gRRTC) and (b) a targeting moiety that has specific binding affinity for a folate receptor. In some embodiments, the targeting moiety has specific binding affinity for folate receptor alpha (FR-a), folate receptor beta (FR-b), and/or folate receptor delta (FR-d). In some embodiments, the targeting moiety has a specific binding affinity for folate receptor alpha (FR-a), folate receptor beta (FR-b), and/or folate receptor delta (FR-d). In some embodiments, the targeting moiety has a specific binding affinity for folate receptor alpha (FR-a) and folate receptor beta (FR-b). In some embodiments, the administered liposomal composition comprises pegylated liposomes (e.g., TPLp-gRRTC). In some embodiments, the administered liposomal composition comprises liposomes that are not pegylated. In some embodiments, liposomes of the administered liposomal composition comprises an gRRTC containing 4, 5, 2-10, 4-6, or more than 5, g-glutamyl groups. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the D-form. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the L-form. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing 2, 3, 4, 5, or more than 5, g-glutamyl groups in the L-form, and 1, 2, 3, 4, 5 or more than 5, g-glutamyl groups in the D-form. In some embodiments, a liposome of the administered liposomal composition comprises gamma pentaglutamated pralatrexate. In other embodiments, a liposome of the administered liposomal composition comprises gamma hexaglutamated pralatrexate. In some embodiments, the liposomal composition is administered to treat a cancer selected from the group consisting of: a non-hematologic malignancy including such as for example, lung cancer, pancreatic cancer, breast cancer, ovarian cancer, prostate cancer, head and neck cancer, gastric cancer, gastrointestinal cancer, colorectal cancer, esophageal cancer, cervical cancer, liver cancer, kidney cancer, biliary duct cancer, gallbladder cancer, bladder cancer, sarcoma (e.g., osteosarcoma), brain cancer, central nervous system cancer, and melanoma; and a hematologic malignancy such as for example, a leukemia, a lymphoma and other B cell malignancies, myeloma and other plasma cell dysplasias or dyscrasias.

[0048] In additional embodiments, the disclosure provides a method for cancer maintenance therapy that comprises administering an effective amount of a liposomal composition comprising liposomes that contain gamma polyglutamated pralatrexate (Lp- gRRTC) to a subject that is undergoing or has undergone cancer therapy. In some embodiments, the administered liposomal composition is a PLp-gRRTC, NTLp-gRRTC, NTPLp-gRRTC, TLp-gRRTC or TPLp-gRRTC. In some embodiments, the administered liposomal composition comprises pegylated liposomes (e.g., PLp-gRRTC, NTPLp-gRRTC, or TPLp-gRRTC). In some embodiments, the administered liposomal composition comprises targeted liposomes (e.g., TLp-gRRTC or TPLp-gRRTC). In some embodiments, the administered liposomal composition comprises liposomes that are pegylated and comprise a targeting moiety (e.g., TPLp-gRRTC). In some embodiments, a liposome of the administered liposomal composition comprises gamma polyglutamated pralatrexate that contains 4, 5, 2-10, 4-6, or more than 5, g-glutamyl groups. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing 1, 2,

3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the D-form. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the L-form. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing 2, 3, 4, 5, or more than 5, g-glutamyl groups in the L-form, and 1, 2, 3,

4, 5 or more than 5, g-glutamyl groups in the D-form. In some embodiments, a liposome of the administered liposomal composition comprises gamma tetraglutamated pralatrexate. In some embodiments, a liposome of the administered liposomal composition comprises gamma pentaglutamated pralatrexate. In other embodiments, a liposome of the administered liposomal composition comprises gamma hexaglutamated pralatrexate.

[0049] In additional embodiments, the disclosure provides a method for treating a disorder of the immune system that comprises administering an effective amount of a liposomal composition comprising liposomes that contain gamma polyglutamated pralatrexate (e.g., Lp-gRRTC, PLp-gRRTC, NTLp-gRRTC, NTPLp-yPPTX, TLp-gRRTC or TPLp-gRRTC) to a subject having or at risk of having a disorder of the immune system. In some embodiments, the liposomal composition is administered to treat an autoimmune disease. In a further embodiment, the liposomal composition is administered to treat rheumatoid arthritis. In another embodiment, the liposomal composition is administered to treat inflammation· In some embodiments, the administered liposomal composition comprises pegylated liposomes (e.g., PLp-gRRTC, NTPLp-gRRTC, or TPLp-gRRTC). In some embodiments, the administered liposomal composition comprises targeted liposomes (e.g., TLp-gRRTC or TPLp-gRRTC) that contain a targeting moiety having a specific affinity for a surface antigen on a target cell of interest (e.g., an immune cell). In further embodiments, the administered liposomal composition comprises liposomes that are pegylated and comprise a targeting moiety (e.g., TPLp-gRRTC)). In some embodiments, a liposome of the administered liposomal composition comprises gamma pentaglutamated pralatrexate that contains 4, 5, 2-10, 4-6, or more than 5, g-glutamyl groups. In some embodiments, a liposome of the administered liposomal composition comprises a gRRTC containing 1, 2,

4, 5 or more than 5, g-glutamyl groups in the D-form. In some embodiments, a liposome of the administered liposomal composition comprise gamma tetraglutamated pralatrexate. In some embodiments, a liposome of the administered liposomal composition comprise gamma pentaglutamated pralatrexate. In other embodiments, liposomes of the administered liposomal composition comprise gamma hexaglutamated pralatrexate.

[0050] The disclosure also provides a method of delivering gamma polyglutamated pralatrexate to a tumor and/or cancer cell that comprises: administering to a subject having the tumor, a composition comprising gamma polyglutamated pralatrexate (L-gRRTC) and a targeting moiety that has a specific binding affinity for an epitope on a surface antigen on the tumor cell or cancer cell. In some embodiments, the administered targeting moiety is associated with a delivery vehicle. In some embodiments, the delivery vehicle is an antibody or an antigen binding fragment of an antibody. In further embodiments, the delivery vehicle is a liposome. In further embodiments, the antibody, antigen-binding antibody fragment, or liposome is pegylated liposomes (e.g., TPLp-gRRTC). In some embodiments, the administered composition comprises gamma polyglutamated pralatrexate that contains 4, 5, 2-10, 4-6, or more than 5, glutamyl groups. In some embodiments, the administered composition comprises gamma tetraglutamated pralatrexate. In some embodiments, the administered composition comprises gamma pentaglutamated pralatrexate. In other embodiments, the administered composition comprises gamma hexaglutamated pralatrexate.

[0051] In additional embodiments, the disclosure provides a method of preparing a liposomal composition that comprises a liposomal gamma polyglutamated pralatrexate (gRRTC) composition, the method comprising: forming a mixture comprising: liposomal components and g polyglutamated pralatrexate in solution; homogenizing the mixture to form liposomes in the solution; and processing the mixture to form liposomes containing polyglutamated pralatrexate. In some embodiments, the gamma polyglutamated pralatrexate contains 4, 5, 2-10, 4-6, or more than 5, g-glutamyl groups. In some embodiments, the gRRTC composition contains 1, 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the D-form. In some embodiments, the gRRTC composition contains 2, 3, 4, 5, 6, 7, 8, 9, 10, or more than 10, g-glutamyl groups in the L-form. In some embodiments, the gRRTC composition contains 2, 3, 4, 5, or more than 5, g-glutamyl groups in the L-form, and 1, 2, 3, 4, 5 or more than 5, g-glutamyl groups in the D-form. In some embodiments, the gRRTC composition comprises gamma pentaglutamated pralatrexate. In some embodiments, the gRRTC composition comprises gamma tetraglutamated pralatrexate. In other embodiments, the gRRTC composition comprises gamma hexaglutamated pralatrexate.

[0052] In one embodiment, the disclosure provides a kit comprising a gamma polyglutamated pralatrexate composition and/or gRRTC delivery vehicles such as liposomes containing gRRTC and gRRTC immunoconjugates (e.g., ADCs) described herein.

BRIEF DESCRIPTION OF THE DRAWINGS/FIGURES

[0001] FIGS. 1A-1L show chemical formulas of pralatrexate (FIG. 1A), exemplary gamma pralatrexate poly glutamates, pralatrexate diglutamate (FIG. IB), pralatrexate triglutamate (FIGS. 1C and ID), pralatrexate tetraglutamate (FIGS. IE and IF), pralatrexate pentaglutamates (FIGS. 1G and 1H), pralatrexate hexaglutamates (FIGS. II and 1J), pralatrexate heptaglutamate (FIGS. IK and 1L), pralatrexate octaglutamates (FIG. 1M and IN), and exemplary gamma pralatrexate polyglutamates (FIG. lO).

[0002] FIG. 2 presents an example dose response relationship of free pemetrexed L- gamma hexaglutamate (gG6), liposomal pemetrexed L-gamma hexaglutamate (liposomal gG6), pemetrexed, and folate receptor alpha targeting antibody (FRlAb) liposomal pemetrexed L-gamma hexaglutamate (liposomal gG6-FRlAb) in the NCI H2342 non small cell lung cancer (NSCLC), adenocarcinoma subtype depicted as the percentage of viable cells after 48 hours of treatment.

[0003] FIG. 3 presents an example dose response relationship of free pemetrexed L- gamma hexaglutamate (gG6), liposomal pemetrexed L-gamma hexaglutamate (liposomal gG6), pemetrexed, and folate receptor alpha targeting antibody (FRlAb) liposomal pemetrexed L-gamma hexaglutamate (liposomal gG6-FRlAb) in the HT-29 (colon cancer) at 48 hours.

[0004] FIG. 4 shows the effect of free pemetrexed L-gamma hexaglutamate (hexa gG6) and liposomal pemetrexed L-gamma hexaglutamate (liposomal hexa gG6), on the growth of colon cancer SW260 cells following exposure of 256 nM of the corresponding agent for 48 hours. The non-targeted and targeted liposomal pemetrexed hexa gG6 are able to enter cells more efficiently than free pemetrexed hexa gG6 to inhibit growth of the colon cancer SW260 cells.

[0005] FIG. 5 presents the relative potency of liposomal pemetrexed L-gamma hexaglutamate (liposomal gG6) and its mirror image, liposomal pemetrexed gamma-D hexaglutamate (liposomal gDG6) relative to pemetrexed following exposure of the cancer cell lines SW620 (CRC), HT-29 (colon cancer), H1806 (triple negative breast cancer), OAW28 (ovarian cancer), H292 (NSCLC, adenocarcinoma subtype), and H2342 (NSCLC, adenocarcinoma subtype), over 48 hours.

[0006] FIG.6 presents the treatment effect on HCC 1806 triple negative breast cancer cells following exposure of liposomal pemetrexed gamma-L hexaglutamate (Lps Hexa gG6), liposomal pemetrexed gamma-D hexaglutamate (Lps Hexa gDG6), and to pemetrexed over 48 hours.

[0007] FIG. 7 presents the treatment effect on OAW28 ovarian cancer cells following exposure of liposomal pemetrexed gamma-L hexaglutamate (Lps Hexa gG6), liposomal pemetrexed gamma-D hexaglutamate (Lps Hexa gDG6), as compared to pemetrexed over 48 hours.

[0008] FIG. 8 presents the treatment effect on H292 non-small cell lung cancer cells following exposure of liposomal pemetrexed gamma-L hexaglutamate (Lps Hexa gG6), liposomal pemetrexed gamma-D hexaglutamate (Lps Hexa gDG6), and to pemetrexed over 48 hours.

[0009] FIG. 9 presents the treatment effect on H292 non-small cell lung cancer cells following exposure of various dose levels ranging from 16 to 128 nM of liposomal pemetrexed gamma-L hexaglutamate (Liposomal gG6), liposomal pemetrexed gamma-D hexaglutamate (Liposomal gDG6), and pemetrexed over 48 hours. At each of the tested dose ranges, the liposomal pemetrexed gG6 formulation is superior to inhibiting H292 non small cell lung cancer cells compared to pemetrexed.

[0010] FIG. 10 presents the treatment effect on HCC1806 triple negative breast cancer cells following exposure of various dose levels ranging from 16 to 128 nM of liposomal pemetrexed gamma-L hexaglutamate (Liposomal gG6), liposomal pemetrexed gamma-D hexaglutamate (Liposomal gDG6), and pemetrexed over 48 hours. At each of the tested doses, the liposomal pemetrexed gG6 formulation is superior to pemetrexed in inhibiting HCC1806 triple negative breast cancer cells.

[0011] FIG. 11 presents the treatment effect on OAW28 ovarian cancer cells of liposomal pemetrexed gamma-L hexaglutamate (LiposomalgG6), liposomal gamma-D hexaglutamate (LiposomalgDG6), and pemetrexed following exposure over 48 hours following exposure over a range of concentrations. At the dose of 128 nM, pemetrexed appears to more effective than the Liposomal pemetrexed gG6 liposomal formulation, whereas the liposomal formulation at the dose of 32 nM and 64 nM has a better treatment effect than pemetrexed; at 16 nM the Liposomal pemetrexed gG6 treatment effect is similar in to pemetrexed.

[0012] FIG. 12 shows the toxicity of liposomal pemetrexed gamma-L hexaglutamate

(LiposomalgG6), liposomal pemetrexed gamma-D hexaglutamate (Liposomal gDG6), and pemetrexed on differentiating human neutrophils at 64 nM, 128 nM, and 264 nM. The figure demonstrates that liposomal pemetrexed gG6 is significantly less toxic to differentiating human neutrophils than pemetrexed. [0013] FIG. 13 shows the effect of liposomal pemetrexed gamma-L hexaglutamate

(liposomalgG6), liposomal gamma-D hexaglutamate (liposomalgDG6), and pemetrexed on on neutrophils (differentiated from CD34+ cells) following exposure of various dose levels ranging from 16 to 128 nM of the corresponding agent over 48 hours.

[0014] FIG. 14 shows the effect of liposomal pemetrexed gamma-L hexaglutamate

(liposomalgG6), liposomal pemetrexed gamma-D hexaglutamate (liposomalgDG6), and pemetrexed on AML12 liver cells following exposure over 48 hours at 16 nM, 32 nM, and 64 nM, and 128 nM of the corresponding agent. Strikingly, there does not appear to be any toxicity to the AML12 liver cells following treatment with a liposomal pemetrexed gG6 at any of the liposomal agents at the dose levels tested. In contrast, pemetrexed treatment results in a reduction in the AML12 liver cell counts of approximately 40% at all doses studied.

[0015] FIG. 15 shows the effect of liposomal pemetrexed gamma-L hexaglutamate

(liposomalgG6), liposomal pemetrexed gamma-D hexaglutamate (liposomalgDG6), and pemetrexed on CCD841 colon epithelium cells following exposure over 48 hours at 16 nM, 32 nM, and 64 nM, and 128 nM, of the corresponding agent. At all of the concentrations tested, pemetrexed leads to approximately a >50% decrease in the number of CCD841 colon epithelium cells compared to approximately a 20% or less decrease in cell number after treatment with each of the liposome compositions tested.

[0016] FIG. 16 depicts the structure of polyglutamate antifolate, Cisplatin (CDDP) and two potential gG6-Cisplatin complexes. The pH dependent formation of the interstrand and/or instrastrand coordination between the carboxyl groups of the polyglutamated antifolate and cisplatin is likely to disassemble into individual molecules of gG6 and cisplatin upon encountering acidic pH of lysosomes (pH 3-5) and presence of chloride ions inside the cells.

[0017] FIG. 17 presents the effects of liposomal aG6 treatment of mice with 40 mg/kg and 80 mg/kg given once weekly for 4 weeks upon the hematologic parameters: white blood cell (WBC) counts, neutrophil counts and as platelet counts. No appreciable decrease in mean neutrophil, mean white blood cell or mean platelet counts was observed.

[0018] FIG. 18 presents the effects of liposomal aG6 treatment of mice with 40 mg/kg and 80 mg/kg given once weekly for 4 weeks upon hemoglobin and reticulocyte indices. There is a minimal decrease in mean hemoglobin concentrations at the higher dose level. In parallel there is a slight increase in mean reticulocytosis indices

[0019] FIG. 19 presents the effects of liposomal aG6 treatment of mice with 40 mg/kg and 80 mg/kg given once weekly for 4 weeks upon hepatic markers including serum aspartate transaminase (AST) and serum alanine transaminase (ALT) along with serum albumin. There was no appreciable increases in liver transaminases mean AST or mean ALT levels and there was no observed change in mean albumin levels.

[0020] FIG. 20 presents the relative tumor volume of immunodeficient female Nu/J mice (6-8 weeks old) inoculated with NCI-H292 (Non-Small Cell Lung Cancer) cells and administered control, pemetexed, and Liposomal aG6 intravenously at 167 mg/kg once every three weeks. As can be seen from these preliminary data, liposomal aG6 provides reduced tumor control compared to pemetrexed.

[0021] FIGS. 21A-F present the dose response relationship of liposomal pemetrexed alpha-L triglutamate (Liposomal aG3), liposomal pemetrexed alpha-L pentaglutamate (Liposomal aG5), liposomal pemetrexed alpha-L octaglutamate (Liposomal aG7), and a combination of liposomal pemetrexed alpha-L hexaglutamate (aG6) and alpha-L dodecaglutamate (aGl2) (Liposomal aG6 and aGl2), over 48 hours on H2342 (NSCLC, adenocarcinoma subtype)(FIG. 21A), H292 (NSCLC, adenocarcinoma subtype)(FIG. 21B), HT-29 (colon cancer)(FIG. 21C), HCC1806 (triple negative breast cancer)(FlG. 21D), MCF7 (ER+ breast cancer)(FIG. 21E), and OAW28 (ovarian cancer)(FIG. 21F). Cell viability was determined by CellTiter-Glo® (CTG) luminescent cell viability assay essentially as described in Example 1. As shown in all cell lines, the potency of each of the polyglutamated pemetrexed liposomal compositions well exceeded that of the liposomal vehicle and empty liposome controls.

DETAILED DESCRIPTION

[0022] The disclosure generally relates to gamma polyglutamated pralatrexate compositions. The compositions provide advances over prior treatments of hyperproliferative diseases such as cancer. Methods of making, delivering and using the gamma polyglutamated pralatrexate compositions are also provided. The gamma polyglutamated compositions have uses that include but are not limited to treating or preventing hyperproliferative diseases such as cancer, disorders of the immune system such as inflammation and rheumatoid arthritis, and infectious disease such as HIV and malaria.

I. Definitions

[0023] Unless defined otherwise, all technical and scientific terms used herein have the same meaning as commonly understood by one of ordinary skill in the art to which the disclosure pertains.

[0024] It is understood that wherever embodiments, are described herein with the

language“comprising” otherwise analogous embodiments, described in terms of “containing”“consisting of’ and/or“consisting essentially of’ are also provided.

However, when used in the claims as transitional phrases, each should be interpreted separately and in the appropriate legal and factual context (e.g., in claims, the transitional phrase“comprising” is considered more of an open-ended phrase while the transitional phrases“consisting of’ is more exclusive and“consisting essentially of’ achieves a middle ground).

[0025] As used herein, the singular form“a”,“an”, and“the”, includes plural references unless it is expressly stated or is unambiguously clear from the context that such is not intended.

[0026] The term“and/or” as used in a phrase such as“A and/or B” herein is intended to include both A and B; A or B; A (alone); and B (alone). Likewise, the term“and/or” as used in a phrase such as“A, B, and/or C” is intended to encompass each of the following embodiments: A, B, and C; A, B, or C; A or C; A or B; B or C; A and C; A and B; B and C; A (alone); B (alone); and C (alone).

[0027] Headings and subheadings are used for convenience and/or formal compliance only, do not limit the subject technology, and are not referred to in connection with the interpretation of the description of the subject technology. Features described under one heading or one subheading of the subject disclosure may be combined, in various embodiments, with features described under other headings or subheadings. Further it is not necessarily the case that all features under a single heading or a single subheading are used together in embodiments.

[0028] Unless indicated otherwise, the terms “pralatrexate” and “PTX” are used interchangeably to include a salt, acid and and/or free base form of pralatrexate (e.g., pralatrexate disodium). Compositions containing a PTX salt may further contain any of a variety of cations, such as Na ⁺, Mg ²⁺, K ⁺, NH ₄ ⁺, and/or Ca ²⁺. In particular embodiments, the salts are pharmaceutically acceptable salts. In additional particular embodiments, the PTX salt contains Na ⁺. Pralatrexate contains one L-gamma glutamyl group, and is therefore considered to be monoglutamated for the purpose of this disclosure. The term pralatrexate is used herein to refer to a racemic mixture of S- and R- diastereomers, and/or a composition containing mostly the S- diastereomer or the R- diastereomer, unless otherwise specififd.

[0029] The terms “polyglutamated-pralatrexate”, “poly glutamated- PTX”, “PTX-PG”,

“PPTX” and iterations thereof, are used interchangeably herein to refer to a pralatrexate composition that comprises at least one glutamyl group in addition to the glutamyl group of pralatrexate (/. _<?., PTX-PG _n, wherein n > 1). Reference to the number of glutamyl groups in an gRRTC (PTX-PG) herein takes into account the glutamyl group of pralatrexate. For example, a PTX-PG composition containing 5 glutamyl residues in addition to the glutamyl group of PTX is referred to herein as hexaglutamated pralatrexate or pralatrexate hexaglutamate. Polyglutamate chains comprise an N-terminal glutamyl group and one or more C-terminal glutamyl groups. The N-terminal glutamyl group of a polyglutamate chain is not linked to another glutamyl group via its amine group, but is linked to one or more glutamyl group via its carboxylic acid group. In some embodiments, the N-terminal glutamyl group of a polyglutamated-tetrahydrofolate is the glutamyl group of pralatrexate. The C-terminal glutamyl group or groups of a polyglutamate chain are linked to another glutamyl group via their amine group, but are not linked to another glutamyl group via their carboxylic acid group.

[0030] The terms“gamma glutamyl group”,“gamma glutamyl group”, and“gamma linkage”, as they relate to the linkage of a glutamyl group, refers to a glutamyl group that contains a gamma carboxyl group linkage. The gamma linkage can be between a glutamyl group and the glutamyl group of pralatrexate, or between a glutamyl group and a second glutamyl group that is not present in pralatrexate (e.g., a glutamyl group within a polyglutamate chain attached to pralatrexate). In some embodiments, the gamma linkage is an amide bond between the gamma carboxyl group of one glutamyl group and a second glutamyl group. In some embodiments, the gamma linkage refers to the amide bond of the glutamyl group in pralatrexate. In some embodiments, the gamma linkage is an amide bond between the gamma carboxyl group of one glutamyl group and a second glutamyl group. Reference to gamma linkages are inclusive of the gamma linkage of the glutamyl group in pralatrexate unless it is expressly stated or is unambiguously clear from the context that such is not intended. In some embodiments, the gamma glutamyl group is in the L-form. In some embodiments, the gamma glutamyl group is in the D-form. As discussed herein, during pralatrexate therapy, pralatrexate enters the cell and is polyglutamated by the enzyme folylpoly-gamma-glutamate synthetase (FPGS), which adds L glutamyl groups serially to the gamma carboxyl group of the glutamate within pralatrexate L-glutamyl group of pralatrexate. Consequently, D-gamma polyglutamated pralatrexate compositions are not formed within cells during pralatrexate therapy.

[0031] The terms “gamma polyglutamated pralatrexate”, “g-polyglutamated pralatrexate”,“gRRTC”,“gamma polyglutamated-pralatrexate”,“polyglutamated-PTX”, “gRTC-PG”, and iterations thereof, are used interchangeably herein to refer to a pralatrexate composition that comprises at least one gamma glutamyl group having a gamma carboxyl group linkage in addition to the gamma glutamyl group of pralatrexate (e.g., PTX-PG _n, wherein n > 1 g glutamyl group). Reference to the number of glutamyl groups in a gRRTC (gRTC-PG) herein takes into account the glutamyl group of pralatrexate. For example, a gRTC-PG composition containing 5 g-glutamyl groups in addition to the glutamyl group of PTX may be referred to herein as gamma hexaglutamated pralatrexate or gamma pralatrexate hexaglutamate.

[0032] The terms“alpha glutamyl group”,“a-glutamyl group”, and“alpha linkage”, as they relate to the linkage of a glutamyl group, refers to a glutamyl group that contains an alpha carboxyl group linkage.

[0033] As use herein, the term“isolated” refers to a composition which is in a form not found in nature. Isolated gamma polyglutamated compositions include those which have been purified to a degree that they are no longer in a form in which they are found in nature. In some embodiments, a gamma polyglutamated pralatrexate which is isolated is substantially pure. Isolated compositions will be free or substantially free of material with which they are naturally associated such as other cellular components such as proteins and nucleic acids with which they may potentially be found in nature, or the environment in which they are prepared (e.g., cell culture). The gamma polyglutamated compositions may be formulated with diluents or adjuvants and still for practical purposes be isolated - for example, the gamma polyglutamated compositions will normally be mixed with phamiaceutically acceptable carriers or diluents when used in diagnosis or therapy. In some embodiments, the isolated gamma polyglutamated compositions (e.g., gamma polyglutamates and delivery vehicles such as liposomes containing the gamma poly glutamate contain less than 1% or less than 0.1% undesired DNA or protein content. In some embodiments, the gamma polyglutamate compositions (e.g., gamma polyglutamate and delivery vehicles such as liposomes containing the gamma poly glutamate) are "isolated."

[0034] The term“targeting moiety” is used herein to refer to a molecule that provides an enhanced affinity for a selected target, e.g., a cell, cell type, tissue, organ, region of the body, or a compartment, e.g., a cellular, tissue or organ compartment. The targeting moiety can comprise a wide variety of entities. Targeting moieties can include naturally occurring molecules, or recombinant or synthetic molecules. In some embodiments, the targeting moiety is an antibody, antigen-binding antibody fragment, bispecific antibody or other antibody-based molecule or compound. In some embodiments, the targeting moiety is an aptamer, avimer, a receptor-binding ligand, a nucleic acid, a biotin-avidin binding pair, a peptide, protein, carbohydrate, lipid, vitamin, toxin, a component of a microorganism, a hormone, a receptor ligand or any derivative thereof. Other targeting moieties are known in the art and are encompassed by the disclosure.

[0035] The terms“specific affinity”,“specifically binds”, and“enhanced affinity”, mean that a targeting moiety such as an antibody or antigen binding antibody fragment, reacts or associates more frequently, more rapidly, with greater duration, with greater affinity, or with some combination of the above to the epitope, protein, or target molecule than with alternative substances, including proteins unrelated to antigens containing the target epitope. Because of the sequence identity between homologous proteins in different species, specific affinity can, in several embodiments, include a binding agent that recognizes an epitope on a protein and/or target molecule in more than one species. Likewise, because of homology within certain regions of polypeptide sequences of different proteins, the term“specific affinity” or“specifically binds” can include a binding agent that recognizes an epitope that is present on more than one protein and/or target molecule. It is understood that, in certain embodiments, a targeting moiety that specifically binds a first target may or may not specifically bind a second target. As such, “specific affinity” does not necessarily require (although it can include) exclusive binding, e.g., binding to an epitope on a single target. Thus, a targeting moiety may, in certain embodiments, specifically bind an epitope that is present on more than one target. In certain embodiments, multiple targets may be bound by the same targeting moiety specifically binds an epitope that is present on multiple targets.

[0036] The term "epitope" refers to that portion of an antigen capable of being

recognized and specifically bound by a targeting moiety (i.e., binding moiety) such as an antibody. When the antigen is a polypeptide, epitopes can be formed both from contiguous amino acids and noncontiguous amino acids juxtaposed by tertiary folding of a protein. Epitopes formed from contiguous amino acids are typically retained upon protein denaturing, whereas epitopes formed by tertiary folding are typically lost upon protein denaturing. An epitope typically includes at least 3, and more usually, at least 5 or 8-10 amino acids in a unique spatial conformation.

[0037] Expressions like“binding affinity for a target”,“binding to a target”,“enhanced affinity”, and analogous expressions known in the art refer to a property of a targeting moiety which may be directly measured through the determination of the affinity constants, e.g., the amount of targeting moiety that associates and dissociates at a given antigen concentration. Different methods can be used to characterize the molecular interaction, such as, but not limited to, competition analysis, equilibrium analysis and microcalorimetric analysis, and real-time interaction analysis based on surface plasmon resonance interaction (for example using a Biacore® instrument). These methods are well- known to the skilled person and are described, for example, in Neri et al., Tibtech 14:465- 470 (1996), and Jansson et al., J. Biol. Chem. 272:8189-8197 (1997).

[0038] The term "delivery vehicle" refers generally to any compositions that acts to assist, promote or facilitate entry of gamma polyglutamated pralatrexate into a cell. Such delivery vehicles are known in the art and include, but are not limited to, liposomes, lipospheres, polymers (e.g., polymer-conjugates), peptides, proteins such as antibodies (e.g., immunoconjugates, such as Antibody Drug Conjugates (ADCs) and antigen binding antibody fragments and derivatives thereof), cellular components, cyclic oligosaccharides (e.g., cyclodextrins), micelles, microparticles (e.g., microspheres), nanoparticles (e.g., lipid nanoparticles, biodegradable nanoparticles, and core-shell nanoparticles), hydrogels, lipoprotein particles, viral sequences, viral material, or lipid or liposome formulations, and combinations thereof. The delivery vehicle can be linked directly or indirectly to a targeting moiety. In some examples, the targeting moiety is selected from among a macromolecule, a protein, a peptide, a monoclonal antibody or a fatty acid lipid.

[0039] A“subject” refers to a human or vertebrate mammal including but not limited to a dog, cat, horse, goat and primate, e.g., monkey. Thus, the invention can also be used to treat diseases or conditions in non-human subjects. For instance, cancer is one of the leading causes of death in companion animals (e.g., cats and dogs). In some embodiments, of the invention, the subject is a human. In this disclosure, the term“subject” and“patient” is used interchangeably and has the same meaning. It is preferred generally that a maximum dose be used, that is, the highest safe dose according to sound medical judgment.

[0040] As used herein an“effective amount” refers to a dosage of an agent sufficient to provide a medically desirable result. The effective amount will vary with the desired outcome, the particular condition being treated or prevented, the age and physical condition of the subject being treated, the severity of the condition, the duration of the treatment, the nature of the concurrent or combination therapy (if any), the specific route of administration and like factors within the knowledge and expertise of the health practitioner. An "effective amount" can be determined empirically and in a routine manner, in relation to the stated purpose. In the case of cancer, the effective amount of an agent may reduce the number of cancer cells; reduce the tumor size; inhibit (/. _<?., slow to some extent and preferably stop) cancer cell infiltration into peripheral organs; inhibit (/. _<?., slow to some extent and preferably stop) tumor metastasis; inhibit, to some extent, tumor growth; and/or relieve to some extent one or more of the symptoms associated with the disorder. To the extent the drug may prevent growth and/or kill existing cancer cells, it may be cytostatic and/or cytotoxic. For cancer therapy, efficacy in vivo can, for example, be measured by assessing the duration of survival, duration of progression free survival (PFS), the response rates (RR), duration of response, and/or quality of life.

[0041] The terms“hyperproliferative disorder”, "proliferative disease", and“proliferative disorder”, are used interchangeably herein to pertain to an unwanted or uncontrolled cellular proliferation of excessive or abnormal cells which is undesired, such as, neoplastic or hyperplastic growth, whether in vitro or in vivo. In some embodiments, the proliferative disease is cancer or tumor disease (including benign or cancerous) and/or any metastases, wherever the cancer, tumor and/or the metastasis is located. In some embodiments, the proliferative disease is a benign or malignant tumor. In some embodiments, the proliferative disease is a non-cancerous disease. In some embodiments, the proliferative disease is a hyperproliferative condition such as hyperplasias, fibrosis (especially pulmonary, but also other types of fibrosis, such as renal fibrosis), angiogenesis, psoriasis, atherosclerosis and smooth muscle proliferation in the blood vessels, such as stenosis or restenosis following angioplasty.

[0042] “Cancer”,“tumor”, or“malignancy”, are used as synonymous terms and refer to any of a number of cell types or diseases that are characterized by uncontrolled, abnormal proliferation of cells, the ability of affected cells to spread locally or through the bloodstream and lymphatic system to other parts of the body (metastasize) and/or any of the characteristic structural and/or molecular features known to be associated with these cell types or diseases.“Tumor”, as used herein refers to all neoplastic cell growth and proliferation, whether malignant or benign, and all pre-cancerous and cancerous cells and tissues. A“cancerous tumor”, or“malignant cell” is understood as a cell having specific structural properties, lacking differentiation and being capable of invasion and metastasis. A cancer that can be treated using an gRRTC composition provided herein includes without limitation, a non-hematologic malignancy including such as for example, lung cancer, pancreatic cancer, breast cancer, ovarian cancer, prostate cancer, head and neck cancer, gastric cancer, gastrointestinal cancer, colorectal cancer, esophageal cancer, cervical cancer, liver cancer, kidney cancer, biliary duct cancer, gallbladder cancer, bladder cancer, sarcoma (e.g., osteosarcoma), brain cancer, central nervous system cancer, and melanoma; and a hematologic malignancy such as for example, a leukemia, a lymphoma and other B cell malignancies, myeloma and other plasma cell dysplasias or dyscrasias. Other types of cancer and tumors that may be treated using an gRRTC composition are described herein or otherwise known in the art. The terms“cancer,” “cancerous,”“cell proliferative disorder,”“proliferative disorder,” and“tumor” are not mutually exclusive as referred to herein.

[0043] Terms such as "treating”, "treatment”, or "to treat", refer to both (a) therapeutic measures that cure, slow down, lessen symptoms of, and/or halt progression of a diagnosed pathologic condition or disorder and (b) prophylactic or preventative measures that prevent and/or slow the development of a targeted disease or condition. Thus, subjects in need of treatment include those already with the cancer, disorder or disease; those at risk of having the cancer or condition; and those in whom the infection or condition is to be prevented. Subjects are identified as“having or at risk of having” cancer, an infectious disease, a disorder of the immune system, a hyperproliferative disease, or another disease or disorder referred to herein using well-known medical and diagnostic techniques. In certain embodiments, a subject is successfully "treated" according to the methods provided herein if the subject shows, e.g., total, partial, or transient amelioration or elimination of a symptom associated with the disease or condition (e.g., cancer, inflammation, and rheumatoid arthritis). In specific embodiments, the terms treating”, or "treatment”, or "to treat", refer to the amelioration of at least one measurable physical parameter of a proliferative disorder, such as growth of a tumor, not necessarily discernible by the patient. In other embodiments, the terms treating”, or "treatment”, or "to treat", refer to the inhibition of the progression of a proliferative disorder, either physically by, e.g., stabilization of a discernible symptom, physiologically by, e.g., stabilization of a physical parameter, or both. In other embodiments, the terms treating”, or "treatment”, or "to treat", refer to the reduction or stabilization of tumor size, tumor cell proliferation or survival, or cancerous cell count. Treatment can be with a g-RRTC composition, alone or in combination with an additional therapeutic agent.

[0044] “Subject”,“patient”, and“animal”, are used interchangeably and refer to

mammals such as human patients and non-human primates, as well as experimental animals such as rabbits, rats, and mice, and other animals. Animals include all vertebrates, e.g., mammals and non-mammals, such as chickens, amphibians, and reptiles.“Mammal” as used herein refers to any member of the class Mammalia, including, without limitation, humans and nonhuman primates such as chimpanzees and other apes and monkey species; farm animals such as cattle, sheep, pigs, goats and horses; domestic mammals such as dogs and cats; laboratory animals including rodents such as mice, rats and guinea pigs, and other members of the class Mammalia known in the art. In a particular embodiment, the subject is a human.

[0045] “Treatment of a proliferative disorder” is used herein to include maintaining or decreasing tumor size, inducing tumor regression (either partial or complete), inhibiting tumor growth, and/or increasing the life span of a subject having the proliferative disorder. In one embodiment, the proliferative disorder is a solid tumor. Such tumors include, for example, lung cancer, pancreatic cancer, breast cancer, ovarian cancer, prostate cancer, head and neck cancer, gastric cancer, gastrointestinal cancer, colorectal cancer, esophageal cancer, cervical cancer, liver cancer, kidney cancer, biliary duct cancer, gallbladder cancer, bladder cancer, sarcoma (e.g., osteosarcoma), brain cancer, central nervous system cancer, and melanoma. In one embodiment, the proliferative disorder is a hematologic malignancy. Such hematologic malignancies include for example, a leukemia, a lymphoma and other B cell malignancies, myeloma and other plasma cell dysplasias or dyscrasias.

[0046] The term "autoimmune disease" as used herein is defined as a disorder that

results from an autoimmune response. An autoimmune disease is the result of an inappropriate and excessive response to a self-antigen. Examples of autoimmune diseases include but are not limited to, Addison’s disease, alopecia areata, ankylosing spondylitis, autoimmune hepatitis, autoimmune parotitis, Crohn's disease, diabetes (Type I), dystrophic epidermolysis bullosa, epididymitis, glomerulonephritis, Graves' disease, Guillain-Barr syndrome, Hashimoto's disease, hemolytic anemia, systemic lupus erythematosus, multiple sclerosis, myasthenia gravis, pemphigus vulgaris, psoriasis, rheumatic fever, inflammation and rheumatoid arthritis, sarcoidosis, scleroderma, Sjogren's syndrome,

spondyloarthropathies, thyroiditis, vasculitis, vitiligo, myxedema, pernicious anemia, and ulcerative colitis, among others.

[0047] The term“therapeutic agent” is used herein to refer to an agent or a derivative thereof that can interact with a hyperproliferative cell such as a cancer cell or an immune cell, thereby reducing the proliferative status of the cell and/or killing the cell. Examples of therapeutic agents include, but are not limited to, chemotherapeutic agents, cytotoxic agents, platinum-based agents (e.g., cisplatin, carboplatin, oxaliplatin), taxanes (e.g., Taxol), etoposide, alkylating agents (e.g., cyclophosphamide, ifosamide), metabolic antagonists (e.g., methotrexate (MTX), 5- fluorouracil gemcitabine, or derivatives thereof), antitumor antibiotics (e.g., mitomycin, doxorubicin), plant-derived antitumor agents (e.g., vincristine, vindesine, Taxol). Such agents may further include, but are not limited to, the anticancer agents trimetrexate, temozolomide, raltitrexed, S-(4- Nitrobenzyl)-6-thioinosine (NBMPR), 6-benzyguanidine (6-BG), bis-chloronitrosourea (BCNU) and camptothecin, or a therapeutic derivative of any thereof. Additional examples of therapeutic agents that may be suitable for use in accordance with the disclosed methods include, without limitation, anti-restenosis, pro- or anti-proliferative, anti-inflammatory, anti-neoplastic, antimitotic, anti-platelet, anticoagulant, antifibrin, antithrombin, cytostatic, antibiotic and other anti -infective agents, anti-enzymatic, anti-metabolic, angiogenic, cytoprotective, angiotensin converting enzyme (ACE) inhibiting, angiotensin II receptor antagonizing and/or cardioprotective agents.“Therapeutic agents” also refer to salts, acids, and free based forms of the above agents.

[0048] As used herein, the term“chemotherapeutic agent” when used in relation to cancer therapy, refers to any agent that results in the death of cancer cells or inhibits the growth or spread of cancer cells. Examples of such chemotherapeutic agents include alkylating agents, antibiotics, antlmetabolitlc agents, plant-derived agents, and hormones. In some embodiments, the chemotherapeutic agent is cisplatin. In some embodiments, the chemotherapeutic agent is carboplatin. In some embodiments, the chemotherapeutic agent is oxaliplatin. In other embodiments, the chemotherapeutic agent is gemcitabine. In other embodiments, the chemotherapeutic agent is doxorubicin.

[0049] The term“antimetabolite” is used herein to refer to a therapeutic agent that inhibits the utilization of a metabolite or a prodrug thereof. Examples of antimetabolites include methotrexate, pralatrexate, 5-fluorouracil, 5 -fluorouracil prodrugs such as capecitabine, 5- fluorodeoxyuridine monophosphate, cytarabine, cytarabine prodrugs such as nelarabine, 5-azacytidine, gemcitabine, mercaptopurine, thioguanine, azathioprine, adenosine, pentostatin, erythrohydroxynonyladenine, and cladribine. Anti-metabolites useful for practicing the disclosed methods include nucleoside analogs, including a purine or pyrimidine analogs. In some embodiments, the gamma polyglutamated pralatrexate compositions are used in combination with an antimetabolite selection from the group consisting of fluoropyrimidine 5-fluorouracil, 5-fluoro-2'-deoxycytidine, cytarabine, gemcitabine, troxacitabine, decitabine, Azacytidine, pseudoisocytidine, Zebularine, Ancitabine, Fazarabine, 6- azacytidine, capecitabine, N4-octadecyl-cytarabine, elaidic acid cytarabine, fludarabine, cladribine, clofarabine, nelarabine, forodesine, and pentostatin, or a derivative thereof. In one example, the nucleoside analog is a substrate for a nucleoside deaminase that is adenosine deaminase or cytidine deaminase. In some examples, the nucleoside analog is selected from among fludarabine, cytarabine, gemcitabine, decitabine and azacytidine or derivatives thereof. In certain embodiments, the antimetabolite is 5-fluorouracil.

[0050] As used herein, a“taxane” is an anti-cancer agent that interferes with or disrupts microtubule stability, formation and/or function. Taxane agents include paclitaxel and docetaxel as well as derivatives thereof, wherein the derivatives function against microtubules by the same mode of action as the taxane from which they are derived. In certain embodiments, the taxane is paclitaxel or docetaxel, or a pharmaceutically acceptable salt, acid, or derivative of paclitaxel or docetaxel. In certain embodiments, the taxane is paclitaxel (TAXOL®), docetaxel (TAXOTERE®), albumin-bound paclitaxel (nab-paclitaxel; ABRAXANE®), DHA-paclitaxel, or PG-paclitaxel.

[0051] The term "pharmaceutically-acceptable carrier" refers to an ingredient in a pharmaceutical formulation, other than an active ingredient, which is nontoxic to a subject. A pharmaceutically acceptable carrier includes, but is not limited to, a buffer, carrier, excipient, stabilizer, diluent, or preservative. Pharmaceutically-acceptable carriers can include for example, one or more compatible solid or liquid filler, diluents or encapsulating substances which are suitable for administration to a human or other subje.

[0052] This disclosure generally relates gamma polyglutamated pralatrexate (PTX) compositions and methods of making and using the compositions to treat diseases including hyperproliferative diseases such as cancer, disorders of the immune system such as rheumatoid arthritis, and infectious disease such as HIV and malaria.

[0053] In some embodiments, the disclosure provides:

[1] a composition comprising a gamma polyglutamated pralatrexate;

[2] the composition of [1], wherein the gamma polyglutamated pralatrexate

comprises 1-10 glutamyl groups having gamma carboxyl group linkages;

[3] the composition of [1] or [2], wherein the gamma polyglutamated pralatrexate contains 4, 5, 2-10, 4-6, or more than 5, glutamyl groups having gamma carboxyl group linkages;

[4] the composition according to any of [l]-[3], wherein the gamma polyglutamated pralatrexate is gamma tetraglutamated pralatrexate;

[5] the composition according to any of [l]-[3], wherein the gamma polyglutamated pralatrexate is gamma pentaglutamated pralatrexate;

[6] the composition according to any of [l]-[3], wherein the gamma polyglutamated pralatrexate is gamma hexaglutamated pralatrexate;

[7] the composition according to any of [l]-[6], wherein

(a) the gamma polyglutamated pralatrexate comprises two or more glutamyl groups in the L-form having gamma carboxyl group linkages, (b) each of the glutamyl groups of the gamma polyglutamated pralatrexate is in the L-form and has a gamma carboxyl group linkage,

pralatrexate is in the D-form and has a gamma carboxyl group linkage,

(d) each of the glutamyl groups of the gamma polyglutamated pralatrexate other than the glutamyl group of pralatrexate is in the D-form and has a gamma carboxyl group linkage, or

(e) the gamma polyglutamated pralatrexate comprises two or more glutamyl groups in the L-form and at least one glutamyl group in the D-form having gamma carboxyl group linkages;

[9] the composition of [5], wherein (a) each of the glutamyl groups is in the L-form and has a gamma carboxyl group linkage or (b) each of the glutamyl groups other than the glutamyl group of pralatrexate is in the D-form and and each of the gluytamyl groups has a gamma carboxyl group linkage;

[11] the composition according to any of [1]-[10], wherein the gamma polyglutamated pralatrexate is polyglutamable by FGPS under standard operating conditions,

[12] a liposomal composition comprising the gamma polyglutamated pralatrexate according to any of [l]-[l l] (Lp-gRRTC);

[13] the Lp-gRRTC composition according to [12], wherein the gamma

polyglutamated pralatrexate comprises two or more glutamyl groups in the L- form;

[14] the Lp-gRRTC composition according to [12] or [13], wherein each of the

glutamyl groups of the gamma polyglutamated pralatrexate is in the L-form; [15] the Lp-gRRTC composition of [12] or [13], wherein at least one of the glutamyl groups of the gamma polyglutamated pralatrexate is in the D-form;

[16] the Lp-gRRTC composition according to any of [12]-[15], wherein the liposome comprises a gamma polyglutamated pralatrexate comprising 1-10 glutamyl groups having gamma carboxyl group linkages;

[17] the Lp-gRRTC composition according to any of [12]-[16], wherein the liposome comprises a gamma polyglutamated pralatrexate containing 4, 5, 2-10, 4-6, or more than 5, glutamyl groups;

[18] the Lp-gRRTC composition according to any of [12]-[17], wherein the liposome comprises gamma tetraglutamated pralatrexate;

[19] the Lp-gRRTC composition according to any of [12]-[17], wherein the liposome comprises gamma pentaglutamated pralatrexate;

[20] the Lp-gRRTC composition according to any of [12]-[17], wherein the liposome comprises gamma hexaglutamated pralatrexate;

[21] the Lp-gRRTC composition according to any of [l2]-[20], wherein the liposome is not pegylated (PyLp-yPPTX);

[22] the Lp-gRRTC composition according to any of [l2]-[20], wherein the liposome is pegylated (PyLp-yPPTX);

[24] the Lp-gRRTC composition according to any of [l2]-[24], wherein the liposome has a diameter in the range of 20 nm to 500 nm;

[25] the Lp-gRRTC composition according to any of [l2]-[24], wherein the liposome has a diameter in the range of 20 nm to 200 nm;

[26] the Lp-gRRTC composition according to any of [l2]-[25], wherein the liposome has a diameter in the range of 80 nm to 120 nm;

[27] the Lp-gRRTC composition according to any of [l2]-[26], wherein the liposome is formed from liposomal components; [28] the Lp-gRRTC composition according to [27], wherein the liposomal components comprise at least one of an anionic lipid and a neutral lipid;

cholesterol-PEG; and cholesterol-maleimide;

[30] the Lp-gRRTC composition according to any of [27] -[29], wherein the liposomal components comprise at least one selected from the group consisting of: DSPE; DSPE-PEG; DSPE-PEG-FITC; DSPE-PEG-maleimide; cholesterol; and HSPC;