COMPOSITIONS AND METHODS FOR CELLULAR DELIVERY

Title:

COMPOSITIONS AND METHODS FOR CELLULAR DELIVERY

Document Type and Number:

WIPO Patent Application WO/2020/236894

Kind Code:

Abstract:

Disclosed herein are amphiphilic polymers and hierarchical structures (e.g., emulsions) comprising said polymer. Also disclosed herein are methods of using the polymers and hierarchical structure disclosed herein.

More Like This:

WO/2010/125276	IMPROVED METHOD FOR PRODUCING AN ACRYLIC ESTER (CO)POLYMER
WO/2021/039799	CURABLE COMPOSITION
JP6522288	Methacrylic resin composition and its molded article

Inventors:

SLETTEN ELLEN M (US)
ESTABROOK DANIEL A (US)
CHAPMAN JOHN O (US)

Application Number:

PCT/US2020/033730

Publication Date:

November 26, 2020

Filing Date:

May 20, 2020

Export Citation:

Click for automatic bibliography generation Help

Assignee:

UNIV CALIFORNIA (US)

International Classes:

C08F20/18; C08F16/06; C08F16/18; C08F22/10; C08F22/38; C08L29/04; C08L33/08; C08L71/02

Domestic Patent References:

WO2009156180A2

2009-12-30

Other References:

DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: 2-propenoic acid, esters, 2-methyl-, methyl ester, homopolymer", XP055762412, retrieved from STN Database accession no. 9011-14-7
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: 2-propenoic acid, esters, ethyl ester, homopolymer", XP055762414, retrieved from STN Database accession no. 9003-32-1
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: 2-propenoic acid, esters, propyl ester", XP055762416, retrieved from STN Database accession no. 925-60-0
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: 2-propenoic acid, esters, 2-methyl-, butyl ester, homopolymer", XP055762418, Database accession no. 9003-63-8
DATABASE Registry 16 November 1984 (1984-11-16), "2- propenoic acid, 2-methyl-,cyclohexyl ester", XP055762422, retrieved from STN Database accession no. 101-43-9
DATABASE Registry [online] 8 January 2016 (2016-01-08), "2-Propenoic acid, 2-methyl-, phenylmethyl ester, homopolymer", XP055762425, Database accession no. 25085-83-0
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: 2- propenoic acid, esters, 2-methyl-, 2-phenylethyl ester, homopolymer", XP055762428, retrieved from STN Database accession no. 28825-60-7
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: 2-propenoic acid, esters, cyclohexyl ester, homopolymer", XP055762431, retrieved from STN Database accession no. 27458-65-7
DATABASE Registry 16 November 1984 (1984-11-16), "2-Propenoic acid, 2-hydroxyethyl ester, homopolymer (CA INDEX NAME)", XP055762433, retrieved from STN Database accession no. 26022-14-0
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: 2-propenoic acid, phenylmethyl ester", XP055762436, retrieved from STN Database accession no. 2495-35-4
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: 1-propene, polymers, homopolymer", XP055762438, retrieved from STN Database accession no. 9003-07-0
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: 1-Butene, homopolymer", XP055762441, retrieved from STN Database accession no. 9003-28-5
DATABASE Registry 11 September 2012 (2012-09-11), "CA Index Name: poly[oxy(l-methyl-2-oxo-l,2-ethanediyl)], alpha-hydro- omega-(2-propyn-l-yloxy", XP055762443, retrieved from STN Database accession no. 1393882-74-0
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: propanoic acid, polymers, 2-hydroxy-, homopolymer", XP055762452, retrieved from STN Database accession no. 26100-51-6
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: poly(oxy-l,2- ethanediyl), alpha-hydro-omega-hydroxy", XP055762455, retrieved from STN Database accession no. 25322-68-3
DATABASE PubChem Compound 27 March 2005 (2005-03-27), "Poly(propylene glycol).", XP055762246, retrieved from National Center for Biotechnology Information Database accession no. 32881
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: ethene, ethoxy-, homopolymer", XP055762459, retrieved from STN Database accession no. 25104-37-4
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: ethenol, homopolymer", XP055762460, retrieved from STN Database accession no. 9002-89-5
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: 2-propen-l-ol, polymers, homopolymer", XP055762462, retrieved from STN Database accession no. 27251-32-7
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name : benzene,2- propen-l-yl-,homopolymer", XP055762463, retrieved from STN Database accession no. 25988-53-8
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name : ethene, methoxy-, homopolymer", XP055762464, retrieved from STN Database accession no. 9003-09-2
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name : 2-Propen-l-amine, homopolymer", XP055762466, retrieved from STN Database accession no. 30551-89-4
DATABASE ChEBI [online] 16 March 2012 (2012-03-16), "IUPAC Name: omega-hydroxypoly[(acetylimino) ethylene", retrieved from Chemical Entities of Biological Interest Database accession no. 53589
DATABASE Registry 8 November 1994 (1994-11-08), "CA Index Name: 2- oxazoleethanol, 4,5-dihydro-2-methyl-, homopolymer", XP055762467, retrieved from STN Database accession no. 158820-10-1
DATABASE Registry 16 November 1984 (1984-11-16), "CA Index Name: oxazole, 2-(1,1-dimethylethyl)-4,5-dihydro-, homopolymer", XP055762468, retrieved from STN Database accession no. 25822-66-6
DATABASE Registry 3 April 2013 (2013-04-03), "CA Index Name: oxazole, 2-(1,1-dimethylethyl)-4,5-dihydro-, polymer with 2-ethyl-4,5-dihydrooxazole, diblock", XP055762469, retrieved from STN Database accession no. 1427005-74-0
MIYAMOTO MASATOSHI, SANO YOSHIYUKI, KIMURA YOSHIHARU, SAEGUSA TAKEO: ""Spontaneous" vinyl polymerization of 2-vinyl-2-oxazolines", MACROMOLECULES, vol. 18, no. 9, 30 September 1985 (1985-09-30), pages 1641 - 1648, XP055761964
KOURTI MARIA-EVGENIA, FEGA EIRINI, PITSIKALIS MARINOS: "Block copolymers based on 2-methyl- and 2-phenyl-oxazoline by metallocene-mediated cationic ring-opening polymerization: synthesis and characterization", POLYMER CHEMISTRY, vol. 7, no. 16, 28 March 2016 (2016-03-28), pages 2821 - 2835, XP055761966, Retrieved from the Internet
KRIEG ANDREAS, WEBER CHRISTINE, HOOGENBOOM RICHARD, BECER C. REMZI, SCHUBERT ULRICH S.: "Block copolymers of poly(2-oxazoline)s and poly(meth) acrylates: a crossover between cationic ring-opening polymerization (CROP) and reversible addition-fragmentation chain transfer (RAFT", ACS MACRO LETTERS, vol. 1, no. 6, 19 June 2012 (2012-06-19), pages 776 - 779, XP055761968, DOI: http://citeseerx.ist.psu.edu/viewdoc/download ? doi= 10.1.1.968.6480&rep=repl&type=pdf
TRÜTZSCHLER ANNE-KRISTIN, LEISKE MEIKE N., STRUMPF MARIA, BRENDEL JOHANNES C., SCHUBERT ULRICH S.: "One-Pot Synthesis of Block Copolymers by a Combination of Living Cationic and Controlled Radical Polymerization", MACROMOLECULAR RAPID COMMUNICATIONS, vol. 40, no. 1, 9 August 2018 (2018-08-09), pages 1800398, XP055761970
MEYER DE ET AL.: "Drug targeting using thermally responsive polymers and local hyperthermia", JOURNAL OF CONTROLLED RELEASE, vol. 74, no. 1-3, 6 July 2001 (2001-07-06), pages 213 - 24, XP004297526, DOI: 10.1016/S0168-3659(01)00319-4
CHUNG JE ET AL.: "Thermo-responsive drug delivery from polymeric micelles constructed using block copolymers of poly (N-isopropylacrylamide) and poly (butylmethacrylate", JOURNAL OF CONTROLLED RELEASE, vol. 62, no. 1-2, 1 November 1999 (1999-11-01), pages 115 - 27, XP004363009, DOI: 10.1016/S0168-3659(99)00029-2
KOLOUCHOVA KRISTYNA, SEDLACEK ONDREJ, JIRAK DANIEL, BABUKA DAVID, BLAHUT JAN, KOTEK JAN, VIT MARTIN, TROUSIL JIRI, KONEFAŁ RAFAŁ, : "Self-assembled thermoresponsive polymeric nanogels for 19F MR imaging", BIOMACROMOLECULES, vol. 19, no. 8, 16 July 2018 (2018-07-16), pages 3515 - 3524, XP055761973
VICTOR R. DE LA ROSA, AN VAN DEN BULCKE, AND RICHARD HOOGENBOOM: "Poly(2-Oxazoline)s: The Versatile Polymer Platform for Biomedicine", MATERIAL MATTERS, vol. 11, no. 3, 31 December 2016 (2016-12-31), pages 1 - 5, XP055744588
FOREMAN M. B., COFFMAN J. P., MURCIA M. J., CESANA S., JORDAN R., SMITH G. S., NAUMANN C. A.: "Gelation of amphiphilic lipopolymers at the air-water interface: 2D analogue to 3D gelation of colloidal systems with grafted polymer chains?", LANGMUIR, vol. 19, no. 2, 21 January 2003 (2003-01-21), pages 326 - 32, XP055761982
DARGAVILLE TIM R., PARK JONG-RYUL, HOOGENBOOM RICHARD: "Poly(2-oxazoline) hydrogels: state-of-the-art and emerging applications", MACROMOLECULARBIOSCIENCE, vol. 18, no. 6, 30 June 2018 (2018-06-30), pages 1 - 15, XP055762206
LUXENHOFER ROBERT, HAN YINGCHAO, SCHULZ ANITA, TONG JING, HE ZHIJIAN, KABANOV ALEXANDER V., JORDAN RAINER: "Poly(2-oxazoline)s as polymer therapeutics", MACROMOLECULAR RAPID COMMUNICATIONS, vol. 33, no. 19, 15 October 2012 (2012-10-15), pages 1613 - 1631, XP055762201, Retrieved from the Internet
FILIPPOV SERGEY K., VERBRAEKEN BART, KONAREV PETR V., SVERGUN DMITRI I., ANGELOV BORISLAV, VISHNEVETSKAYA NATALYA S., PAPADAKIS CH: "Block and gradient copoly(2-oxazoline) micelles: strikingly different on the inside", THE JOURNAL OF PHYSICAL CHEMISTRY LETTERS, vol. 8, no. 16, 17 August 2017 (2017-08-17), pages 3800 - 3804, XP055762197, Retrieved from the Internet
FUSTIN CHARLES-ANDRÉ, THIJS-LAMBERMONT HANNEKE M. L., HOEPPENER STEPHANIE, HOOGENBOOM RICHARD, SCHUBERT ULRICH S., GOHY JEAN-FRANÇ: "Multiple micellar morphologies from tri-and tetrablock copoly (2-oxazoline)s in binary water-ethanol mixtures", JOURNAL OF POLYMER SCIENCE PART A: POLYMER CHEMISTRY, vol. 48, no. 14, 15 July 2010 (2010-07-15), pages 3095 - 3102, XP055762194
IVANOVA RUZHA, KOMENDA THOMAS, BONNÉ TUNE B., LÜDTKE KARIN, MORTENSEN KELL, PRANZAS P. KLAUS, JORDAN RAINER, PAPADAKIS CHRISTINE M: "Micellar Structures of Hydrophilic/Lipophilic and Hydrophilic/Fluorophilic Poly(2-oxazoline) Diblock Copolymers in Water", MACROMOLECULAR CHEMISTRY AND PHYSICS, vol. 209, no. 21, 6 November 2008 (2008-11-06), pages 2248 - 2258, XP055762192
LEGROS CAMILLE, DE PAUW-GILLET MARIE-CLAIRE, TAM KAM CHIU, TATON DANIEL, LECOMMANDOUX SÉBASTIEN: "Crystallisation-driven self-assembly of poly (2-isopropyl-2-oxazoline)-block- poly (2-methyl-2-oxazoline) above the LCST", SOFT MATTER, vol. 11, no. 17, 9 March 2015 (2015-03-09), pages 3354 - 3359, XP055762190
SAHN MARTIN, STAFAST LEANNE M., DIRAUF MICHAEL, BANDELLI DAMIANO, WEBER CHRISTINE, SCHUBERT ULRICH S.: "LCST behavior of poly (2-ethyl-2-oxazoline) containing diblock and triblock copolymers", EUROPEAN POLYMER JOURNAL, vol. 100, 1 March 2018 (2018-03-01), pages 57 - 66, XP055762187
ZHOU YUANYUAN, WU PEIYI: "Block length-dependent phase transition of poly (N-isopropylacrylamide)-b- poly (2-isopropyl-2-oxazoline) diblock copolymer in water", POLYMER, vol. 153, 26 September 2018 (2018-09-26), pages 250 - 261, XP055762186
SHIEH MING-JIUM, PENG CHENG-LIANG, CHIANG WEI-LUN, WANG CHAU-HUI, HSU CHIA-YEN, WANG SHIAN-JY JASSY, LAI PING-SHAN: "Reduced skin photosensitivity with meta-tetra(hydroxyphenyl) chlorin-loaded micelles based on a poly (2-ethyl-2-oxazoline)-b-poly(d,l-lactide) diblock copolymer in vivo", MOLECULAR PHARMACEUTICS, vol. 7, no. 4, 2 August 2010 (2010-08-02), pages 1244 - 1253, XP055762184
SALGARELLA ALICE RITA, ZAHORANOVÁ ANNA, ŠRÁMKOVÁ PETRA, MAJERČÍKOVÁ MONIKA, PAVLOVA EWA, LUXENHOFER ROBERT, KRONEK JURAJ, LACÍK IG: "Investigation of drug release modulation from poly(2-oxazoline) micelles through ultrasound", SCIENTIFIC REPORTS, vol. 8, no. 1, 2 July 2018 (2018-07-02), pages 1 - 13, XP055762181, Retrieved from the Internet
ESTABROOK DANIEL A., ENNIS AMANDA F., DAY RACHAEL A., SLETTEN ELLEN M.: "Controlling nanoemulsion surface chemistry with poly (2-oxazoline) amphiphiles", CHEMICAL SCIENCE, vol. 10, no. 14, 27 February 2019 (2019-02-27), pages 3994 - 4003, XP055762179, Retrieved from the Internet
BRAZEL CS ET AL.: "Pulsatile local delivery of thrombolytic and antithrombotic agents using poly (N-isopropylacrylamide-co-methacrylic acid) hydrogels", JOURNAL OF CONTROLLED RELEASE, vol. 39, no. 1, 1 March 1996 (1996-03-01), pages 57 - 64, XP000583521, DOI: http://citeseerx.ist.psu.edu/viewdoc/download?doi=10.1.1.384.3406&rep=repl&type=pdf
CAMILLE LEGROS: "Engineering of poly(2-oxazoline)s for potential use in biomedical applications", PH.D. THESIS, 2 April 2015 (2015-04-02), pages 46 - 54, XP055762176, Retrieved from the Internet
See also references of EP 3973003A4

Attorney, Agent or Firm:

HALSTEAD, David P. et al. (US)

Download PDF:

View/Download PDF PDF Help

Claims:

CLAIMS We claim: 1. A polymer comprising repeat units represented by formula Ia, formula Ib, formula Ic, formula Id, formula Ie, formula If, formula Ig, or formula Ih:

wherein:

R¹ is a group that imparts hydrophilic character to the polymer;

R² is a group that imparts hydrophobic character to the polymer;

Y¹, Y², Y³, Y⁴, Y⁵, Y⁶, Y⁷, Y⁸, Y⁹, Y¹⁰, and Y¹¹ are each independently selected from NR³, O, or S, Se, P, C(R³)2 each R³ is independently selected from hydrogen, alkyl, and aralkyl;

each R⁴, R⁵, R⁶, R⁷, R⁸, R⁹, R¹⁰, R¹¹, R¹², and R¹³ is independently selected from hydrogen, alkyl (e.g., perfluoroalkyl, perfluoroalkylalkyl, or heteroalkyl), cycloalkyl, arylalkyl, heteroaryl, and heterocyclyl;

hydrogen, alkyl, and aralkyl;

u is an integer from 1 to 10; and

v is an integer from 1 to 10. 2. The polymer of claim 1, wherein the polymer comprises repeat units represented by formula Ia or formula Ih:

wherein:

R¹ is a group that imparts hydrophilic character to the polymer;

R² is a group that imparts hydrophobic character to the polymer;

Y¹ and Y² are independently selected from NR³, O, or S;

each R³ is independently selected from hydrogen, alkyl, and aralkyl;

u is an integer from 1 to 10; and

v is an integer from 1 to 10. 3. The polymer of claim 1, wherein the polymer comprises repeat units represented by at least formula Ia and formula Ih:

wherein:

R¹ is a group that imparts hydrophilic character to the polymer;

R² is a group that imparts hydrophobic character to the polymer;

Y¹ and Y² are independently selected from NR³, O, or S;

each R³ is independently selected from hydrogen, alkyl, and aralkyl;

u is an integer from 1 to 10; and

v is an integer from 1 to 10. 4. The polymer of claim 1, wherein the polymer is represented by formula Ia or formula Ih:

wherein:

R¹ is a group that imparts hydrophilic character to the polymer;

R² is a group that imparts hydrophobic character to the polymer; Y¹ and Y² are independently selected from NR³, O, or S;

each R³ is independently selected from hydrogen, alkyl, and aralkyl;

u is an integer from 1 to 10; and

v is an integer from 1 to 10. 5. The polymer of any one of claims 1-3, wherein the polymer comprises a block W and a block X wherein:

block W comprises at least one repeat unit of formula Ib, formula Ic, formula Id, formula Ie, or formula If, formula Ig; and

block X comprises at least one repeat unit of formula Ib. 6. The polymer of any one of claims 1-3, wherein the polymer comprises a block W and a block X wherein:

block W comprises at least one repeat unit of formula Ia; and

block X comprises at least one repeat unit of formula Ib. 7. The polymer of any one of claims 1-4, wherein the polymer comprises a block W and a block X wherein:

block W comprises at least one repeat unit of formula Ib, formula Ic, formula Id, formula Ie, formula If, or formula Ig; and

block X comprises at least one repeat unit of formula Ih. 8. The polymer of any one of claims 1-4, wherein the polymer comprises a block W and a block X wherein:

block W comprises at least one repeat unit of formula Ia; and

block X comprises at least one repeat unit of formula Ih. 9. The polymer of any one of claims 5-9, wherein block W comprises from 1 to 500 repeat units. 10. The polymer of any one of claims 5-9, wherein block W comprises 30 repeat units. 11. The polymer of any one of claims 5-9, wherein block W comprises 90 repeat units.

12. The polymer of any one of claims 5-10, wherein block X comprises from 1 to 50 repeat units. 13. The polymer of any one of claims 5-10, wherein block X comprises 10 repeat units. 14. The polymer of any one of claims 5-13, wherein the polymer contains more than one block of W. 15. The polymer of any one of claims 5-14, wherein the polymer contains more than one block of X. 16. The polymer of any one of claims 5-15, wherein the ratio of blocks W:X is from about 1:1 to about 20:1. 17. The polymer of any one of claims 5-16, wherein the ratio of blocks W:X is from about 1:1 to about 5:1. 18. The polymer of any one of claims 5-17, wherein the ratio of blocks W:X is about 3:1. 19. The polymer of any one of claims 5-16, wherein the ratio of blocks W:X is about 9:1. 20. The polymer of any one of claims 5-15, wherein the ratio of blocks X:W is about 1:1 to about 5:1. 21. The polymer of any one of claims 5-13, wherein the polymer contains one block of W and one block of X. 22. The polymer of any one of claims 6-19, wherein W contains 30 repeat units and X contains 10 repeat units. 23. The polymer of any one of claims 5-22, wherein W comprises 30 repeat units and X comprises 10 repeat units.

24. The polymer of any one of claims 5-22, wherein W comprises 90 repeat units and X comprises 10 repeat units. 25. The polymer of any one of claims 5-22, wherein W comprises about 30 repeat units and X comprises about 10 repeat units. 26. The polymer of any one of claims 5-22, wherein W comprises about 90 repeat units and X comprises about 10 repeat units. 27. The polymer of any one of claims 1-26, wherein the ratio of repeat units comprising a hydrophilic group to repeat units comprising a hydrophobic group is from about 2:1 to about 20:1. 28. The polymer of any one of claims 1-27, wherein the ratio of repeat units comprising a hydrophilic group to repeat units comprising a hydrophobic group is about 3:1. 29. The polymer of any one of claims 1-27, wherein the ratio of repeat units comprising a hydrophilic group to repeat units comprising a hydrophobic group is about 9:1. 30. The polymer of any one of claims 1-29, wherein the polymer is represented by formula II:

wherein:

n is an integer from 1 to 500; and

m is an integer from 1 to 500. 31. The polymer of claim 30, wherein n is about 30.

32. The polymer of claim 30, wherein n is about 90. 33. The polymer of any one of claims 30-32, wherein m is about 10. 34. The polymer of claim 30, wherein the ratio of n:m is about 3:1. 35. The polymer of claim 30, wherein the ratio of n:m is about 9:1. 36. The polymer of any one of claims 1-35, wherein the polymer further comprises an end group L selected from a nucleophile, a biomolecule, or a polymer chain (e.g., polyethylene glycol chain). 37. The polymer of claim 36, wherein the polymer is represented by formula III:

38. The polymer of any one of claims 1-37, wherein Y¹ is oxygen. 39. The polymer of any one of claims 1-38, wherein Y² is oxygen. 40. The polymer of any one of claims 1-39, wherein R¹ is C₁-C₃ alkyl. 41. The polymer of any one of claims 1-39, wherein R¹ is methyl, ethyl, or isopropyl. 42. The polymer of any one of claims 1-39, wherein R¹ is alkenyl (e.g., vinyl or allyl). 43. The polymer of any one of claims 1-39, wherein R¹ is sulfonylalkyl. 44. The polymer of any one of claims 1-39, wherein R¹ is hydroxyalkyl.

45. The polymer of any one of claims 1-44, wherein R² is C3-C20alkyl. 46. The polymer of any one of claims 1-44, wherein R² is n-propyl, butyl, octyl, or nonyl. 47. The polymer of any one of claims 1-44, wherein R² is C₄-C₂₀fluoroalkyl (e.g., C₄- C₂₀perfluoroalkyl or C₄-C₂₀perfluoroalkylalkyl). 48. The polymer of any one of claims 1-44, wherein R² is tridecafluorooctanyl. 49. The polymer of any one of claims 1-44, wherein R² is cycloalkyl. 50. The polymer of any one of claims 1-44, wherein R² is aryl. 51. The polymer of any one of claims 1-50, wherein u is 1. 52. The polymer of any one of claims 1-50, wherein v is 1. 53. The polymer of any one of claims 1-52, wherein the polymer further comprises a block Z and Z is a repeat unit represented by formula IV:

wherein:

Y³ selected from NR³, O, or S;

R⁴ is a linking moiety (e.g., a precursor to a click reaction); and

i is an integer from 1 to 10. 54. The polymer of claim 53, wherein the linking moiety is capable of participating in a 1,3-dipolar cycloaddition reaction, a hetero-diels reaction, a nucleophilic substitution reaction, a non-aldol type carbonyl reaction, an oxidation reaction, or a click reaction.

55. The polymer of claim 53 or 54, wherein the linking moiety is capable of participating in a click reaction. 56. The polymer of any one of claims 53-55, wherein R⁴ is alkenyl (e.g., butenyl). 57. The polymer of any one of claims 53-55, wherein R⁴ is alkynyl (e.g., ethynyl). 58. The polymer of any one of claims 53-57, wherein Y³ is oxygen. 59. The polymer of any one of claims 53-45, wherein i is 1. 60. The polymer of any one of claims 53-59, wherein Z comprises from 1 to 90 repeat units. 61. The polymer of any one of claims 53-60, wherein Z comprises from 1 to 30 repeat units. 62. The polymer of any one of claims 53-61, wherein the polymer contains one block of Z. 63. The polymer of any one of claims 53-61, wherein the polymer contains more than one block of Z. 64. The polymer of any one of claims 36-63, wherein L is a biomolecule (e.g., a protein). 65. The polymer of any one of claims 46-63, wherein L is a nucleophile. 66. The polymer of any one of claims 46-63, wherein L is amino, hydroxyl, carboxyl, amido, thio, sulfonyl, or sulfoxyl. 67. The polymer of any one of claims 1-66, wherein the polymer is capable of forming hierarchical structures. 68. A plurality of polymers of any one of claims 1-67.

69. The composition of claim 68, wherein the plurality of polymers has a number average of repeat units in W from 1 to 500. 70. The composition of claim 68 or 69, wherein the plurality of polymers has a number average of repeat units in W of about 30. 71. The composition of claim 68 or 69, wherein the plurality of polymers has a number average of repeat units in W of about 90. 72. The composition of any one of claims 68-71, wherein the plurality of polymers has a number average of repeat units in X from 1 to 50. 73. The composition of any one of claims 68-71, wherein plurality of polymers has a number average of repeat units in X of about 10. 74 The composition of claim 68 or 69, wherein the plurality of polymers has a number average of repeat units in W of about 30 and a number average of repeat units in X of about 10. 75 The composition of claim 68 or 69, wherein the plurality of polymers has a number average of repeat units in W of about 90 and a number average of repeat units in X of about 10. 76. The composition of any one of claims 68-75, wherein, based on a number average, the ratio of repeat units comprising a hydrophilic group to repeat units comprising a hydrophobic group is from about 2:1 to about 20:1. 77. The composition of any one of claims 68-76, wherein, based on a number average, the ratio of repeat units comprising a hydrophilic group to repeat units comprising a hydrophobic group is about 3:1. 78. The composition of any one of claims 68-76, wherein, based on a number average, the ratio of repeat units comprising a hydrophilic group to repeat units comprising a hydrophobic group is about 9:1.

79. A hierarchical structure comprising a thermoresponsive polymer, wherein the hierarchical structure has a lower critical solution pH, a lower critical solution osmolarity, a lower critical macromolecule concentration, and/or a lower critical solution temperature (LCST). 80. A hierarchical structure comprising the polymer of any one of claims 1-67. 81. A hierarchical structure comprising the composition of any one of claims 68-78. 82. The hierarchical structure of any one of claims 79-81, wherein the hierarchical structure is an emulsion. 83. The hierarchical structure of any one of claims 79-82, wherein the hierarchical structure is a nanoemulsion. 84. The hierarchical structure of any one of claims 79-58, wherein the hierarchical structure is a liposome. 85. The hierarchical structure of any one of claims 79-84, wherein the hierarchical structure is a micelle. 86. The hierarchical structure of any one of claims 79-85, wherein the hierarchical structure is from about 10 nm to about 500 nm in diameter. 87. The hierarchical structure of any one of claims 79-86, wherein the hierarchical structure is from about 20 nm to about 500 nm in diameter. 88. The hierarchical structure of any one of claims 79-87, wherein the hierarchical structure is about 120 nm, about 130 nm, about 140 nm, about 150 nm, about 160 nm, about 170 nm, about 180 nm, about 190 nm, about 200 nm, about 210 nm, about 220 nm, about 230 nm, about 240 nm, about 250 nm, about 260 nm, about 270 nm, about 280 nm, about 290 nm, about 300 nm, about 310 nm, about 320 nm, about 330 nm, about 340 nm, about 350 nm, about 360 nm, about 370 nm, about 380 nm, about 390 nm, about 400 nm, about 410 nm, about 420 nm, about 430 nm, about 440 nm, about 450 nm, about 460 nm, about 470 nm, about 480 nm, about 490 nm or about 500 nm in diameter. 89. The hierarchical structure of any one of claims 79-88, wherein the hierarchical structure is about 185 nm in diameter. 90. The hierarchical structure of any one of claims 79-89, wherein the hierarchical structure further comprises at least one active agent. 91. The hierarchical structure of claim 90, wherein the active agent is covalently coupled to the polymer. 92. The hierarchical structure of claim 90 or 91, wherein the active agent is covalently coupled to the surface of the hierarchical structure. 93. The hierarchical structure of claim 90, wherein the active agent is not covalently coupled to the polymer. 94. The hierarchical structure of any one of claims 90-93, wherein the hierarchical structure encapsulates the active agent. 95. The hierarchical structure of any one of claims 90-94, wherein the hierarchical structure enmeshes the active agent. 96. The hierarchical structure of any one of claims 79-95, wherein the active agent is selected from a small molecule, a protein (e.g., an antibody), a polynucleotide, and an imaging agent. 97. The hierarchical structure of any one of claims 79-96, wherein the hierarchical structure has a lower critical solution pH, a lower critical solution osmolarity, a lower critical macromolecule concentration, or LCST. 98. The hierarchical structure of claim 97, wherein the hierarchical structure has a lower critical solution pH.

99. The hierarchical structure of claim 97, wherein the hierarchical structure has a lower osmolarity. 100. The hierarchical structure of claim 97, wherein the hierarchical structure has a lower critical macromolecule concentration. 101. The hierarchical structure of claim 97, wherein the hierarchical structure has a LCST. 102. The hierarchical structure of claim 100, wherein the lower critical macromolecule concentration at about 37°C is from about 70 to about 250 mg/mL. 103. The hierarchical structure of claim 101, wherein the LCST of the hierarchical structure is from about 30°C to about 70°C under the conditions present in a physiologic fluid or in a cell. 104. The hierarchical structure of claim 103, wherein the LCST of the hierarchical structure is about 35°C, about 37.5°C, about 40°C, about 42.5°C, about 45°C, about 47.5°C, about 50°C, about 52.5°C, about 55°C, 57.5°C, or about 60°C under the conditions present in a physiologic fluid or in a cell. 105. The hierarchical structure of claim 103 or 104, wherein the LCST under the conditions present in a physiologic fluid, such as blood, is below 37°C. 106. The hierarchical structure of claim 103 or 104, wherein the LCST under the conditions present in a physiologic fluid, such as blood, is above 37°C. 107. The hierarchical structure of claim 105 or 106, wherein the physiological fluid is an extracellular physiological fluid. 108. The hierarchical structure of claim 101, wherein the LCST under the conditions present inside a cell is above 37°C. 109. The hierarchical structure of claim 101, wherein the LCST under the conditions present inside a cell is below 37°C.

110. The hierarchical structure of any one of claims 79-109, wherein the hierarchical structure comprises an internal hydrophilic phase. 111. The hierarchical structure of any one of claims 79-109, wherein the hierarchical structure comprises an internal hydrophobic phase. 112. The hierarchical structure of any one of claims 79-109, wherein the hierarchical structure comprises an internal fluorous phase. 113. The hierarchical structure of any one of claims 79-109, wherein the external surface of the hierarchical structure is hydrophilic. 114. The hierarchical structure of any one of claims 79-109, wherein the external surface of the hierarchical structure is hydrophobic. 115. A pharmaceutical composition comprising the polymer or hierarchical structure of any one of claims 1-114 and an active agent. 116. A pharmaceutical composition comprising the polymer, composition, or hierarchical structure of any one of claims 1-114 and an active agent. 117. A method of delivering a bioactive agent to an interior of a cell, comprising contacting the cell with the polymer or hierarchical structure of any one of claims 1-114. 118. A method of delivering a bioactive agent to an interior of a cell, comprising contacting the cell with the polymer, composition, or hierarchical structure of any one of claims 1-114. 119. The method of claim 117 or 118, wherein the method comprises contacting the cell with the hierarchical structure of any one of claims 80-114. 120. The method of any one of claims 117-119, wherein the step of contacting the cell comprises administering the pharmaceutical composition of claim 113 to a subject (e.g., a human).

121. The method of any one of claims 117-120, wherein the hierarchical structure degrades after entering the interior of the cell. 122. A method of administering a bioactive agent to subject, comprising administering to the subject the polymer, hierarchical structure, or pharmaceutical composition of any one of claims 1-116. 123. A method of administering a bioactive agent to subject, comprising administering to the subject the polymer, composition, hierarchical structure, or pharmaceutical composition of any one of claims 1-116. 124. A polymer, composition, or hierarchal structure of any one of claims 1-116 for use as a medicament. 125. Use of a polymer, composition, or hierarchal structure of any one of claims 1-116 in the manufacture of a medicament.

Description:

COMPOSITIONS AND METHODS FOR CELLULAR DELIVERY GOVERNMENT SUPPORT

This invention was made with government support under Grant Number GM067555, awarded by the National Institutes of Health. The government has certain rights in the invention.

RELATED APPLICATIONS

This application claims the benefit of U.S. Provisional Patent Application No.

62/850,514, filed on May 20, 2019. The contents of this application are hereby incorporated by reference in their entirety.

BACKGROUND

Hierarchical structure (e.g., micelle, vesicle, nanoparticle and nanoemulsion) formulations can improve the pharmaceutical properties of a biotherapeutic (e.g., a drug) by, for example, enhancing circulation half-life and facilitating the accumulation in a target tissue. Compared to conventional approaches, formulations of hierarchical structures can protect antigen/adjuvant payloads from the surrounding biological environment, thus increasing their half-life and minimizing their systemic toxicity. A critical advantage of the said formulations is the release of the payload at the desired site. Previously, approaches such as changes in pH or redox potential, the presence of an enzyme, or externally applied stimuli (light, heat, ultrasounds, magnetic field) are have been employed. However, to date, there are no formulations that respond to changes in macromolecule concentration, such as those that occur upon entry into a cell or other physical region where macromolecules are present at a higher concentration than in physiological fluids. Thus, there is an unmet need and accordingly, new formulations that respond to changes in macromolecule concentration are required. SUMMARY OF THE INVENTION

In certain aspects, the present disclosure provides polymers comprising repeat units represented by formula Ia, formula Ib, formula Ic, formula Id, formula Ie, formula If, formula Ig, or formula Ih:

wherein:

R ¹ is a group that imparts hydrophilic character to the polymer;

R ² is a group that imparts hydrophobic character to the polymer;

Y ¹, Y ², Y ³, Y ⁴, Y ⁵, Y ⁶, Y ⁷, Y ⁸, Y ⁹, Y ¹⁰, and Y ¹¹ are each independently selected from NR ³, O, or S, Se, P, C(R ³) ₂

each R ³ is independently selected from hydrogen, alkyl, and aralkyl;

each R ⁴, R ⁵, R ⁶, R ⁷, R ⁸, R ⁹, R ¹⁰, R ¹¹, R ¹², and R ¹³ is independently selected from hydrogen, alkyl (e.g., perfluoroalkyl, perfluoroalkylalkyl, or heteroalkyl), cycloalkyl, arylalkyl, heteroaryl, and heterocyclyl;

hydrogen, alkyl, and aralkyl;

u is an integer from 1 to 10; and v is an integer from 1 to 10.

In certain aspects, the present disclosure provides hierarchical structures comprising the polymers disclosed herein.

In certain aspects, the present disclosure provides pharmaceutical compositions comprising the polymers and/or hierarchical structures disclosed herein and at least one pharmaceutically acceptable excipient. BRIEF DESCRIPTION OF THE DRAWINGS FIG.1A depicts the formation of a hierarchical structure comprising poly(2- oxazoline) (POx) shell, an internal phase, and a payload (e.g., a bioactive agent).

FIG.1B depicts the response of a hierarchical structure (e.g., a POx nanoparticle) to environment changes, such as an increase in temperature. As the temperature increases, the hierarchical structure degrades, thereby releasing its payload (e.g., a bioactive agent).

FIG.1C depicts how polymer chains (e.g., POx polymer chains) change

configuration in response to an increase or decrease in temperature.

FIG.1D depicts the internalization of a hierarchical structure (e.g., a POx

nanoparticle) by a cell. When the hierarchical structure enters an environment containing a high concentration of salts, the hierarchical structure degrades, thereby releasing its payload (e.g., a bioactive agent).

FIG.2A shows the lower critical solution temperature (LCST) of a POx polymer. The LCST of the polymer is approximately 50°C.

FIG.2B shows the average size of hierarchical structures disclosed herein (e.g., POx nanoparticles). The average size of the hierarchical structure is approximately 200 nm.

FIG.2C shows the LCST of a EtOx ₃₀-b-ButOx ₁₀-t-OH hierarchical structure . The LCST of the polymer is approximately 55°C.

FIG.2D shows the change in fluorescence as an EtOx30-b-ButOx10-t-OH hierarchical structure degrades and releases its payload. As the hierarchical structure degrades, the fluorescence decreases.

FIG.2E shows minimal change in fluorescence as an MeOx30-b-NonOx10-t-OH (a surfactant lacking LCST) hierarchical structure does not degrade and does not release its payload following heating. Consequently, fluorescence does not decrease. This is a control for the experiment depicted in FIG.2D FIG.3 shows the change in the LCST of both a POx hierarchical structure (e.g., a nanoemulsion) vs. a control polymer. As the concentration of BSA increase, the LCST of the hierarchical structure decreases.

FIG.4 shows the results of a panel of amphiphilic surfactants with varying hydrophilic and hydrophobic blocks, along with changes in block length. Me =–CH3, Et =– C ₂H ₅, Bu =–C ₄H ₉, Non =–C ₉H ₁₉. Polymer in solution (micelles) LCST determined by measuring turbidity through a UV-vis spectrometer with temperature control, where a sudden increase in absorbance (or decrease in transmittance) accompanies the LCST transition.

LCST-induced degradation of PFOB nanoemulsions was measured through DLS with temperature control, tracking size changes versus 5 °C temperature increments.

FIG.5 shows the characterization of the LCST for polymeric micelles composed of either P(EtOx)90-b-P(NonOx)10 or P(MeOx)90-b-P(NonOx)10, dissolved in PBS at 5 mg/mL. Analyzed via UV-Vis spectrometry with temperature control at 2 °C increments.

FIG.6 shows the characterization of the LCST for perfluorooctylbromide

nanoemulsions stabilized by either P(EtOx)90-b-P(NonOx)10 or P(MeOx)90-b-P(NonOx)10. Analyzed via Dynamic light scattering with temperature control at 5 °C increments.

FIG.7 shows the characterization of the LCST for perfluorooctylbromide

nanoemulsions stabilized by P(EtOx)90-b-P(NonOx)10 in the presence of varying

concentrations of BSA (0–250 mg/mL). For comparison to physiological fluids (e.g. blood), human serum (containing ~52 mg/mL of human serum albumin) and fetal bovine serum (containing ~36 mg/mL of bovine serum albumin) are included. When the hydrophilic block is altered to P(MeOx)90, there is still no observable LCST up to 65 °C, even in the presence of BSA (100 mg/mL).

FIG.8 shows that phase separation is observed for nanoemulsions only when (i) stabilized by P(EtOx)90-b-P(NonOx)10, (ii) in the presence of BSA (100 mg/mL), and (iii) heated to 37 °C. Lower layer = perfluorooctylbromide, upper layer = PBS + BSA.

FIG.9 shows that microscopic phase separation at increased concentrations of BSA in PBS (250 mg/mL) is observed PFOB nanoemulsions stabilized by polymeric surfactant were injected directly into a PBS +/- BSA solution and directly imaged using an

epifluorescence microscope (scale bars: 200 mM).

FIG.10 is a plot of the LCST (°C) versus crowding agent (mg/mL) for both (i) free polymer P(EtOx)90-b-P(NonOx)10 in solution (i.e. hierarchical structure = micelles) and (ii) PFOB emulsions stabilized by P(EtOx) ₉₀-b-P(NonOx) ₁₀.“Release window” is determined as temperature below that of physiological temperature (37 °C) and above the crowding expected in a physiological fluid (~80 mg/mL).

FIG.11 is a plot of aggregation concentration (mg/mL) versus molecular weight for a series of poly(ethylene glycol) (PEG) additives. Aggregation concentration is defined as the minimum concentration of PEG that is needed to induce demulsification of P(EtOx)90-b- P(NonOx) ₁₀ stabilized PFOB nanoemulsions at room temperature (25 °C).

FIG.12 shows the results of serial dilutions of P(EtOx) ₉₀-b-P(NonOx) ₁₀-stabilized PFOB emulsions in PBS (pH 7.4). Droplet diameters (nm) were tracked versus temperature (°C) for each diluted solution, from 20 to 70 °C, using dynamic light scattering.

FIG.13 shows the dependence of LCST on pH for P(EtOx) ₉₀-b-P(NonOx) ₁₀- stabilized PFOB emulsions in PBS. Solutions were pH’d using 0.5 mM NaOH or HCl.

FIG.14 is a plot of normalized absorbance (au) traces versus temperature (°C) for micellar P(EtOx) ₉₀-b-P(NonOx) ₁₀ in the presence of either macromolecular crowding agent Ficoll-400 (0-250 mg/mL) or control monomer sucrose (250 mg/mL). Compared to equal concentrations of Ficoll-400 crowder, monomeric sucrose has a negligible influence on the LCST, showing the significance of macromolecular crowding.

FIG.15 is a plot of size (nm) versus temperature (°C) for P(EtOx) ₉₀-b-P(NonOx) ₁₀ stabilized PFOB nanoemulsions in the presence of either macromolecular crowding agent PEG-10k (25.0 mg/mL) or equimolar 18-crown-6 (0.7 mg/mL), capable of making the same number of hydrogen bonds to neighboring water molecules. Compared to equimolar PEG- 10k, 18-crown-6 additive has a negligible influence on emulsion degradation temperature, indicating that the mechanism of LCST reduction is not competition for hydration water.

FIG.16 is a plot of polydispersity index (PDI) versus temperature (°C) for P(EtOx) ₉₀- b-P(NonOx)10 stabilized PFOB nanoemulsions in the presence of either macromolecular crowding agent PEG-10k, or small molecule viscogen ethylene glycol (EG). Compared to an equally viscous solution composed of PEG-10k, a viscous solution of EG increases the LCST, showing that the decrease in LCST is not attributable to changes in viscosity. DETAILED DESCRIPTION OF THE INVENTION

The lower critical solubility temperature (LCST) of a polymer denotes the

temperature at which a polymer undergoes a random coil-to-globule transition. In aqueous media, below this temperature polymers remain soluble; above this temperature, polymers transition to an insoluble, globular state. The LCST can be affected by both intrinsic and extrinsic factors which influence entropic or enthalpic effects including, but not limited to, solvent, polymer hydrophilic-lipophilic balance (HLB), and additives (e.g. salt or

macromolecules).

Amphiphilic polymers, such as poly(2-oxazoline)s (POx), are a class of biocompatible surfactants that possess a wide range of chemistries, such as tunable lower critical solution temperature (LCST) and the ability to form self-assembled nanostructures and stabilize nanoemulsions (NEs). Furthermore, the LCST of a hierarchical structure formed from certain polymers (e.g., POx) may be altered in response to certain environmental changes, such as pH, salt concentration, and/or macromolecule concentration.

The LCST of hierarchical structures formed from certain polymers, such as poly(2- oxazoline)s, poloxamers, acrylates, methacrylates, or polyamides, may be exploited to induce aggregation at high concentrations of macromolecules, such as those found inside the cell.. Polymers can be designed such that at low concentrations (e.g. <50 mg/mL) of protein, the LCST remains below physiological temperature (37°C). However, at high concentrations (e.g. >250 mg/mL) of protein, the LCST is reduced below 37 °C, and the poly(2-oxazoline) amphiphiles aggregate. As the concentration of macromolecules in cellulo is orders of magnitude higher than in extracellular matrices (a phenomenon known as the

macromolecular crowding effect), this change in macromolecular crowding can be used as a trigger to affect polymeric assemblies in cellulo.

Higher-order stimuli-responsive hierarchical structures (e.g., micelles, vesicles, nanoparticles, or nanoemulsions) may be constructed to exploit these phenomena. When soluble, poly(2-oxazoline) amphiphiles disclosed herein act as effective surfactants for forming such structures, and stability is imparted by unfavorable polymer-polymer mixing interactions between polymer-coated emulsions, causing emulsion-emulsion repulsion.

However, upon an LCST transition, polymer-polymer mixing is favorable, which causes de- emulsification. This may occur, for example, via a coalescence mechanism. Such emulsions degrade rapidly in high concentrations of macromolecules (e.g. >250 mg/mL).

Accordingly, the hierarchical structures disclosed herein respond to physiologically relevant stimulus and have many applications, for instance as delivery systems in the cosmetic, food, and pharmaceutical industries.

In one aspect, the present disclosure provides polymers comprising repeat units represented by formula Ia, formula Ib, formula Ic, formula Id, formula Ie, formula If, formula Ig, or formula Ih:

wherein:

R ¹ is a group that imparts hydrophilic character to the polymer;

R ² is a group that imparts hydrophobic character to the polymer;

Y ¹, Y ², Y ³, Y ⁴, Y ⁵, Y ⁶, Y ⁷, Y ⁸, Y ⁹, Y ¹⁰, and Y ¹¹ are each independently selected from NR ³, O, or S, Se, P, C(R ³) ₂

each R ³ is independently selected from hydrogen, alkyl, and aralkyl;

each R ⁴, R ⁵, R ⁶, R ⁷, R ⁸, R ⁹, R ¹⁰, R ¹¹, R ¹², and R ¹³ is independently selected from hydrogen, alkyl (e.g., perfluoroalkyl, perfluoroalkylalkyl, or heteroalkyl), cycloalkyl, arylalkyl, heteroaryl, and heterocyclyl;

hydrogen, alkyl, and aralkyl;

u is an integer from 1 to 10; and v is an integer from 1 to 10.

Typically, the polymers disclosed herein comprise repeat units (e.g., monomers) in a range of configurations. For example, the polymer may contain only one type of repeat units. Alternatively, the polymer may contain more than one type of repeat unit (e.g., 2, 3, 4, or 5 types of repeat units). When the polymer contains more than one type of repeat unit, the repeat units may be arranged in contiguous blocks (e.g., -A-A-A-A-B-B-B-B-), alternating blocks (e.g., -A-A-A-A-B-B-B-B-A-A-A-A-) or the arrangement of the repeat units may be random (e.g., -A-B-B-A-B-A-A-). In certain embodiments, the polymers disclosed herein comprise from 1 to 500 repeat units.

In certain embodiments, the polymer comprises repeat units represented by formula Ia or formula Ih:

wherein:

R ¹ is a group that imparts hydrophilic character to the polymer;

R ² is a group that imparts hydrophobic character to the polymer;

Y ¹ and Y ² are independently selected from NR ³, O, or S;

each R ³ is independently selected from hydrogen, alkyl, and aralkyl;

u is an integer from 1 to 10; and

v is an integer from 1 to 10.

In certain embodiments, the polymer comprises repeat units represented by formula Ia and formula Ih:

wherein:

R ¹ is a group that imparts hydrophilic character to the polymer;

R ² is a group that imparts hydrophobic character to the polymer;

Y ¹ and Y ² are independently selected from NR ³, O, or S;

each R ³ is independently selected from hydrogen, alkyl, and aralkyl;

u is an integer from 1 to 10; and

v is an integer from 1 to 10.

In certain embodiments, the polymer consists essentially of repeat units represented by formula Ia and formula Ih:

wherein:

R ¹ is a group that imparts hydrophilic character to the polymer;

R ² is a group that imparts hydrophobic character to the polymer;

Y ¹ and Y ² are independently selected from NR ³, O, or S; each R ³ is independently selected from hydrogen, alkyl, and aralkyl;

u is an integer from 1 to 10; and

v is an integer from 1 to 10.

In certain embodiments, the polymer is represented by formula Ia or formula Ih:

wherein:

R ¹ is a group that imparts hydrophilic character to the polymer;

R ² is a group that imparts hydrophobic character to the polymer;

Y ¹ and Y ² are independently selected from NR ³, O, or S;

each R ³ is independently selected from hydrogen, alkyl, and aralkyl;

u is an integer from 1 to 10; and

v is an integer from 1 to 10.

In certain embodiments, the polymer comprises a block W and a block X wherein: block W comprises at least one repeat unit of formula Ib, formula Ic, formula Id, formula Ie, formula If, or formula Ig; and

block X comprises at least one repeat unit of formula Ih.