KOLB, Hartmuth, C. (6413 Pacific Avenue, Playa Del Rey, CA, 90293, US)
WALSH, Joseph, C. (831 Galloway St, Pacific Palisades, CA, 90272, US)
GANGADHARMATH, Umesh, B. (3714 Bagley Avenue, Apt. #6Los Angeles, CA, 90034, US)
KOLB, Hartmuth, C. (6413 Pacific Avenue, Playa Del Rey, CA, 90293, US)
WALSH, Joseph, C. (831 Galloway St, Pacific Palisades, CA, 90272, US)
| What is claimed is: 1. A method for synthesizing an F-labeled probe the method comprising: a step of eluting an amount of 18F with a first solvent which comprises a predetermined amount of water and at least one organic solvent, the 18F eluting as an 18F solution; and a step of using the 18F solution to perform 18F -labeling in the presence of at least one labeling reagent and at least one phase transfer catalyst so as to generate the 18F -labeled probe; wherein there is no step of drying the 18F starting from a time when the eluting step is performed and ending at a time when the 18F-labeling step is performed. 2. The method of Claim 1; wherein the first solvent further comprises the at least one labeling reagent and the at least one phase transfer catalyst. 3. The method of Claim 1; wherein a total amount of water in the 18F solution is in a range of about 0.1 % to about 5.0 %. 4. The method of Claim 1; wherein the 18F-labeling step includes combining the 18F solution with a probe precursor so as to arrive at an 18F-labeling solution with a total amount of water in a range of about 0.1 % to about 2.0 %. 5. The method of Claim 4; wherein the 18F-labeling step further includes diluting at least one of the 18F solution and the probe precursor with an organic solvent so that, when the 18F solution and the probe precursor are combined, the 18F-labeling solution has the total amount of water in the range of about 0.1 % to about 2.0 %. 6. The method of Claim 1; wherein the at least one labeling reagent is selected from the group consisting of K2C03, KHC03, Cs2C03, potassium mesylate, potassium oxylate, and tetrabutylammonium bicarbonate. 7. The method of Claim 1; wherein the at least one phase transfer catalyst is Kryptofix K222. 8. The method of Claim 1; wherein the organic solvent includes a polar aprotic solvent. 9. The method of Claim 8; wherein the polar aprotic solvent is selected from the group consisting of acetonitrile, dimethyl sulfoxide ("DMSO"), tetrahydrofuran ("THF"), dimethylformamide ("DMF"), N-methylpyrrolidone ("NMP"), and dioxane. 10. The method of Claim 1; wherein the organic solvent includes a polar protic solvent. 11. The method of Claim 10; wherein the polar protic solvent is selected from the group consisting of tBuOH and t-amyl alcohol. 12. The method of Claim 1; wherein the 18F-labeled probe generate is selected from the group consisting of 18F-FDG, 18F-HX4, 18F-FLT, 18F-MISO, 18F-FAZA, 18F-Fallypride, 18F-FHBG, 18F-FHPG, 18F-4-fiurobenzaldehyde, 18F-4-fiuoroethylbenzoate, 18F-4-fluoromethyl benzoate, 18F- fluoroethylazide, and 18F-W372. 13. The method of Claim 1; wherein the 18F-labeled probe generate is 18F-VM4-037. 14. A solution for use in synthesizing an 18F-labeled probe, the solution comprising: an amount of 18F; water; and at least one organic solvent; wherein a total amount of water in the solution is in a range of about 0.1 % to about 5.0 %. 15. The solution of Claim 13, further comprising: at least one labeling reagent; and at least one phase transfer catalyst. 16. The solution of Claim 14, further comprising: a probe precursor; wherein the total amount of water in the solution is in a range of about 0.1 % to about 2.0 %. |
SOLVENTS
[0001] The present application claims priority from Provisional U.S. Patent Application
No. 61/322,074 filed on April 8, 2010, the disclosure of which is incorporated herein by reference in its entirety.
BACKGROUND OF THE INVENTION [0002] 1. Field of the Invention
[0003] The present invention relates to synthesis of 18 F-labeled probes for positron emission tomography ("PET"). More specifically, a method of synthesizing 18 F-labeled probes is disclosed, where a solvent with a predetermined amount of water in at least one organic solvent is used to a) elute the 18 F-fluoride from an anion exchange cartridge and b) perform the 18 F-labeling, without drying the 18 F-fluoride, in the presence of at least one labeling reagent and at least one phase transfer catalyst.
[0004] 2. Description of Related Art.
[0005] Synthesis of 18 F-labeled probes for positron emission tomography ("PET") has increased tremendously over the last 10 years as there is a growing demand for radiopharmaceuticals that successfully detect aberrant biochemical functions in vivo. The unique physiochemical properties of PET tracers make them ideally suited for several imaging applications such as the early detection and staging of diseases, treatment monitoring and stratification of patients who may or may not respond to a particular therapy. ^
[0006] The synthesis of these radiolabeled molecules is undoubtedly time consuming, labor intensive and randomly unreliable. In an effort to minimize these production issues, radiochemists have attempted to reduce the labeling procedures to their simplest, quickest and most reliable protocols. Despite these process improvements, the radiolabeling processes still contain inherent inefficiencies that would benefit from further chemistry and process improvements. [0007] The conventional means for 18 F-labeling involves the formation of "activated" or
"naked" fluoride, i.e. fluoride that is sufficiendy moisture-free and thus suitable for radiolabeling. It is widely known that the desolvation of fluoride increases its nucleophilic character. See V M. Vlasov, "Fluoride ion as a nucleophile and a leaving group in aromatic nucleophilic substitution reactions", J. of Fluorine Chem., vol. 61, pp. 193-216 (1993). In these conventional labeling protocols, trace amounts of 18 F-fluoride are sequestered onto an anion exchange column from several milliliters of 18 0-water. Afterwards, the 18 F-fluoride ion is eluted from the anion exchange column through the use of salts, such as K J CO J , dissolved in water. An additive such as the potassium crown ether Kryptofix K222, which is dissolved in anhydrous acetonitrile, may be used in conjunction with aqueous K^CO j to facilitate the elution of 18 F-fluoride, or optionally added into the reaction vessel after the KjCO j -mediate elution. After the elution step, there is an extensive drying protocol needed as reagents K J CO J and Kryptofix K222 are in a highly hydrous solution of acetonitrile. This drying step generates an activated mixture of K j CC^, Kryptofix K222 and 18 F-fluoride. The drying process begins by evaporating the azeotropic mixture at elevated temperatures, oftentimes at reduced pressures to aid in the evaporation of water from the reaction vessel. This initial drying can take up to 30 minutes to complete, depending on the efficiency of drying. After the first evaporation, it may be necessary to perform additional evaporations to effectively remove of enough water to render the 18 F-fluoride sufficiendy moisture-free for labeling.
[0008] There are several inherent problems with this approach to generating activate reagents for 18 F-fluorination. First, the amount of water present after the initial drying step will vary from run to run given mechanical differences in vacuum, gas flows, valve integrity and temperature control. Any single mechanical problem, or combination thereof, will negatively impact the efficiency of drying and hence, the labeling results. Since the amount of residual water could vary gready from run to run, the radiolabeling results would then be inconsistent, making reliable production of radiotracers difficult. Also, given the time needed to successfully dry the fluoride, a good portion of the total synthesis time is dedicated to the drying step. Lasdy, because of the concern of residual water in the reaction, there is a potential for operators to "overdry" the reaction mixture prior to fluorination. In this instance, drying the reagents for too long may be as equally hurtful as under-drying the reagents (under-drying being the failure to remove sufficient moisture from the reagents for l8 F-fluorination). For example, Kryptofix K222 decomposition is directly related to drying times and temperatures: prolonged drying at high temperature compromises the integrity and functionality of Kryptofix K222. To address these issues, a method that minimizes the length of drying and can accurately control the amount of moisture from run to run would be a substantial improvement to current radiolabeling practices.
[0009] Alternate methods have been developed in an attempt to obviate the need for the drying step that either elute 8 F-fluoride from anion exchange resins using additives in either anhydrous organic solvents (such as acetonitrile, see Joel Aerts et al., "Fast production of highly concentrated reactive [ 18 F] fluoride for aliphatic and aromatic nucleophilic radiolabeling", Tetrahedron Letters, vol. 51, pp. 64-66 (2009); International Patent Application Pub. No. WO 2009/003251) or by using ionic liquids in hydrous acetonitrile (Hyung Woo Kim et al., "Rapid synthesis of [ 18 F]FDG without an evaporation step using an ionic liquid", Applied Radiation and Isotopes, vol. 61, pp. 1241-1246 (2004)). For these types of elutions using compounds with unknown toxicities, one would want to assay for these additives in the final product prior to injection and imaging, which ultimately complicates the production workflow
[0010] The use of hydroalcoholic (i.e. protic solvents) co-mixtures is reported to
improve 18 F-labeling yields over the standard single solvent 18 F-labeling conditions. Dong Wook Kim et al., "A New Class of S N 2 Reactions Catalyzed by Protic Solvents: Facile Fluorination for Isotopic Labeling of Diagnostic Molecules", J. Am. Chem. Soc, vol. 128, no. 50, pp. 16394-16397 (Nov. 23, 2006). While the increases in yields are believed to be a result of the unique interactions between the 18 F-fluoride and possibly the leaving group on the precursor, it is not practical to use hydroalcoholic solvents, such as t-amyl alcohol, as they must be analyzed in the final product. Additionally, the low polarity of these bulky solvents can hinder the precursor's solubility which can be used for the labeling reaction, thus negatively impacting the radiolabeling yield.
SUMMARY OF THE INVENTION
[0011] An ideal process for labeling would include an additive that benefits the labeling yields, requires no additional testing beyond what is currendy in place for tracer production, eliminates the need for the drying step and allows for the precise amount of water to be present in each reaction for every run.
[0012] With this in mind, one embodiment of the current inventions includes a method for synthesizing an 18 F-labeled probe. The method includes a step of eluting an amount of 18 F with a first solvent which includes a predetermined amount of water and at least one organic solvent. In this step, the ,8 F elutes as an 18 F solution. The method also includes a step of using the 18 F solution to perform 18 F-labeling in the presence of at least one labeling reagent and at least one phase transfer catalyst so as to generate the 1 8 F-labeled probe. In the method, there is no step of drying the 18 F starting from a time when the eluting step is performed and ending at a time when the ,8 F-labeling step is performed.
[0013] A solution for use in synthesizing an 18 F-labeled probe is also provided. The solution includes an amount of 18 F, water, and at least one organic solvent. The total amount of water in this solution is in a range of about 0.1 % to about 5.0 %. The solution may also include at least one labeling reagent, and at least one phase transfer catalyst. In addition, the solution may include a probe precursor, and have a total amount of water in a range of about 0.1 % to about 2.0 %.
BRIEF DESCRIPTION OF THE DRAWINGS
[0014] Figure 1 shows an example of fluorodeoxyglucose ( ,8 F) ("FDG" or " 18 F-FDG") synthesis (run number 1) radio thin layer chromatography ("Radio-TLC") of the crude product after fluorination. Rgn 1 is 18 F-fluoride, Rgn 2 is 18 F-FDG, Rgn 3 is an unknown , 8 F-labeled by-product, Rgn 4 is tetra-acetyl 18 F-FDG;
[00 5] Figure 2 shows an example of 18 F-FDG synthesis (run number 2) Radio-TLC of the crude product after fluorination. Rgn 1 is 18 F-fluoride, Rgn 2 is tetra-acetyl 18 F- FDG;
[0016] Figure 3 shows an example of Radio-TLC of the purified 18 F-FDG as measured by Radio-TLC. The purity of ,8 F-FDG is greater than 98%.; [0017] Figure 4 shows an example of [ ,8 F]-fluorodeoxythymidine (" ,8 F-FLT") synthesis,
Radio-TLC of the crude product after fluorination. Rgn 1 is ,8 F-fluoride, Rgn 2 is Bis- Boc 18 F-FLT;
[0018] Figure 5 shows an example of 18 F-FLT synthesis, radio high-pressure liquid chromatography ("Radio-HPLC") of the crude product after hydrolysis. Peaks 2 and 3 are 18 F-fluoride, Peak 4 is ,8 F-FLT.;
[0019] Figure 6 shows [ ,8 F]-3-Huoro-2-(4-((2-niteo-lH-imidazol-l -yl)methyl)-lH-l ,2,3- triazol-l-yl)propan-l-ol (" 18 F-HX4") synthesis, Radio-HPLC of the crude product after hydrolysis. Peak 1 is 18 F-fluoride, Peak 2 is a mixture of ,8 F-HX4 and 18 F-HX4-acetate;
[0020] Figure 7 shows 18 F-HX4 synthesis, Radio-HPLC of the crude product after 18 F- fluorination. Peak 1 is 18 F-fluoride, Peak 2 is 18 F-HX4-OAc; and
[0021] Figure 8 shows l8 F-HX4 synthesis, Radio-HPLC of the crude product after deprotection. Peak 1 is 18 F-fluoride generated by radiolysis, Peak 2 is 18 F-HX4 and Peak 3 is 18 F-HX4-OAc. Peak 1 was not considered in calculating the conversion of 18 F-HX4- OAc into ¾ ,8 F-HX4..
DETAILED DESCRIPTION OF EMBODIMENTS
[0022] It is to be understood that the figures and descriptions of the present invention have been simplified to illustrate elements that are relevant for a clear understanding of the present invention, while eliminating, for purposes of clarity, many other elements which are conventional in this art. Those of ordinary skill in the art will recognize that other elements are desirable for implementing the present invention. However, because such elements are well known in the art, and because they do not facilitate a better understanding of the present invention, a discussion of such elements is not provided herein.
[0023] The present invention will now be described in detail on the basis of exemplary embodiments. [0024] In this invention, 1 F-labeling occurs in high yields with precisely controlled amounts of water without the use of a lengthy drying step. More specifically, a solvent of a predetermined amount of water in at least one organic solvent is used to a) elute the 1 8 F-fluoride from an anion exchange resin and b) perform the ,8 F-labeling, without drying the 18 F-fluoride, in the presence of at least one labeling reagent and at least one phase transfer catalyst. Any suitable labeling reagents and phase transfer catalysts may be used. Examples of appropriate labeling reagents include, K 2 C0 3 , KHC0 3 , Cs 2 C0 3 , potassium mesylate, potassium oxylate, and tetrabutylammonium bicarbonate, An example of a suitable phase transfer catalyst includes Kryptofix K222. The organic solvent may include a polar aprotic solvent, such as, for example, acetonitrile, dimethyl sulfoxide ("DMSO"), tetrahydrofuran ("THF"), dimethylformamide ("DMF"), N-methylpyrrolidone ("NMP"), and dioxane, as well as others. The organic solvent may also include a polar protic solvent, such as, for example, tBuOH and t-amyl alcohol, as well as others.
[0025] The amount of water as a percentage of the total solvent may range from about
0.1% to about 2%. Water, for elution from the anion exchange cartridge however, may range from about 0.1% to about 5%. The amount of base (e.g., K J CO J ) may be about 0.1 to about 50 mg/ mL. Because the amount of water is controlled by the elution of fluoride, the percentage of water remains the same from run to run, making the radiochemistry more consistent. Also, because the fluorination appears to tolerate the presence of a small range of water, there is no need to dry the fluoride. As a beneficial consequence of eliminating the drying step, the decomposition of temperature-sensitive reagents such as Kryptofix K222 and tetrabutylammonium bicarbonate ("TBAB") are minimized. Additionally, the reactions are completed in a shorter period of time, leading to higher yields and more usable product in-hand. There is less mechanical wear on the instrument, since a portion of mechanical system is no longer used for drying. Unlike losses of radioactivity commonly reported as a consequence of drying 18 F-fluoride, this method would not suffer from this type of radioactivity loss. Lasdy, there are fewer chances of labeling failures due to a consistent amount of water always present in every reaction.
[0026] Examples of 18 F-labeled PET probes that can be generated by the method of the present invention include, but are not limited to, [ 18 F]-3-Fluoro-2-(4-((2-nitro-lH- imidazol-l-y^methy^-lH-l^.S-triazol-l-y^propan-l-ol ("HX4" or " 18 F-HX4"), fluorodeoxymymidine ("FLT"), l-[ 18 F]fluoro-3-(2-mlio-lH-irnidazol-l-yl)propan-2-ol ("F-MISO"), [ 18 F]-fluoroazomycinarabinofuranoside ("FAZA"), 5-[3-( ,8 F)fluoropropyl]- 2,3-dmiethoxy-N-{[(2S)-l-(prop-2-en-l-yl)pyrrolidin-2-yl]met hyl}benz amide
("Fallypride"), 9-(4-[ 18 F]Huoro-3-hydroxymemylbutyl)guanine ("FHBG"), 9-[(3-[ ,8 F]- fluoro-l-hyciroxy-2-propoxy)methyl]guanine ("FHPG"), ( 18 F)fluoroethyl azide,
, 8 F-4-flurobenzaldehyde, ,8 F-4-fluoroethylbenzoate, 18 F-4-fluoromethyl benzoate, and 7- Methoxy-2 (6-[ 18 F]fluoropyridin-3-yl)irriidazo[2,l-b]-8-pyridinothiazo le (" 18 F-W372"). Other examples of ,8 F-labeled PET probes that can be generated by the method of the present invention include, but are not limited to, 2'-Deoxy-2'-[ 18 F]fluoro-5-fluoro-l-p-D- arabinofuranos luracil ("FFAU"), as well as the compounds Usted in the table below:
[0027] Without intention of being bound by a particular mechanism or theory, the 18 F- fluoride anion may displace a leaving group, which may include, but is not limited to, tosylates, mesylates, triflates, nosylates, brosylates, trialkylammonium salts, sulfonate esters, halogens and nitro-groups with ,8 F-fluoride in solvents containing the presence of about 0.1% to about 2.0% water. *
[0028] In general, the process for generating the 18 F-labeled probe includes loading an amount of 18 F onto an anion exchange cartridge. By anion exchange cartridge, what is meant is any vessel containing any convenient anion exchange resin or other material suitable for adsorbing 18 F. The 18 F loaded on the anion exchange resin is then prepared for elution. This preparation may include washing the cartridge with an organic solvent (e.g., anhydrous acetonitrile) and then drying the cartridge (e.g., by passing an inert gas through the cartridge.
[0029] Next the ,8 F is eluted from the cartridge, for example by passing a solution
including water, an organic solvent, a labeling reagent, and a phase transfer catalyst through the cartridge so as to obtain an 18 F solution containing 18 F, water, the organic solvent, the labeling reagent, and the phase transfer catalyst. At this point the amount of water in the 18 F solution may range from 0.1 % to 5.0 %. A probe precursor is then combined with the 18 F solution so as to arrive at an 18 F-labeling solution which has water in an amount of from 0.1% to 2.0%. This can be accomplished, for example, by diluting either the probe precursor or the 18 F solution, or both, with an appropriate amount of organic solvent. Accordingly, it is possible to generate the 18 F-labeling solution without any drying of the eluted 18 F solution.
[0030] While the ,8 F-labeling solution should contain water in an amount of from 0.1% to 2.0%, it is preferable for the water to be in an amount of from 0.5 % to 1.5 %, and more preferable for the water to be in an amount of around 1.0 %.
[0031] EXAMPLES:
[0032] Summary of Labeling Results:
**Denotes analysis performed by Radio-HPLC
[0033] Preparation of the K O j and Kryptofix K222 Elution Solvent:
[0034] K 2 C0 3 (11 mg) was dissolved in water (0.1 mL). Kryptofix K222 (100 mg) was dissolved in acetonitrile (1.9 mL). The solutions were mixed and 0.4 mL, or 2 x 0.2 mL, was used to elute 18 F-fluoride from an anion exchange cartridge. [0035] Loading and Drying of the Anion Exchange Cartridge:
[0036] An activated anion exchange cartridge (QMA lite, bicarbonate form), was loaded with 18 F-fluoride in ls O-water. The cartridge was then washed with anhydrous acetonitrile (3 x 1 mL) to remove residual moisture from the cartridge. The cartridge was then further dried by passing an inert gas (such as He) through the cartridge for approximately 30 to 90 seconds.
[0037] Elution of ^F-fluoride From the Anion Exchange Cartridge:
[0038] After a solution of 18 F-fluoride (up to 50 mCi per run) in ls O-water was passed through the ion-exchange column, a solution of K222 (0.4 mL or 2 x 0.2 mL) was passed through the anion exchange cartridge into a dried reaction vessel. An additional portion of anhydrous acetonitrile (0.6 mL) was added to the reaction vessel. This final step constitutes the formation of 18 F-fluoride in a hydrous organic solution that was suitable for radiolabeling.
[0039] Synthesis of 18 F-FDG (Entries 1. 2 and 3):
FDG precursor Tetraacetyl FDG
[0040] Fluorodeoxyglucose ( 18 F) ("FDG" or " ,8 F-FDG") precursor (mannose triflate, 50 mg) dissolved in acetonitrile (1.0 mL) was added to the reaction vessel containing the activated 18 F-fluoride. The reaction is heated at 90°C for 45 seconds.
Radio thin layer chromatography ("Radio-TLC") indicated that the percent conversion of 18 F-fluoride to 18 F-FDG tetraacetate plus 18 F-FDG was >95% (Figure 1). This reaction sequence was repeated a second time and the percent conversion of 18 F-fluoride to ,8 F-FDG tetraacetate plus 18 F-FDG was >95% (Figure 2). When the labeling was performed in a solution containing 5% water (Entry 3), no labeling was observed. [0041] Synthesis of 18 F-FDG (Entry 4V
FDG precursor Tetraacetyl FDG FDG
[0042] FDG precursor (mannose triflate, 50 mg) dissolved in acetonitrile (1.0 mL) was added to the reaction vessel containing the activated 18 F-fluoride (985 mCi). The reaction is heated at 90°C for 45 seconds. The MeCN was removed under reduced pressure and heat. HC1 (2M, 1 mL) was added and the reaction was heated at 100°C for 480 seconds. The crude reaction mixture was diluted with water and passed through a series of cartridges (A1203, CI 8, ICH-HC0 3 ) to afford 445 mCi (60% yield, decay corrected) 65 minutes after EOB. Radio-TLC indicated that purity of ,8 F-FDG was >95% (Figure 3).
[0043] Synthesis of 18 F-FLT (Entry 5):
FLT Precursor Di-boc FLT
"BocBocNos"
FLT
[0044] Fluorodeoxythymidine ( 18 F) ("FLT" or " 18 F-FLT") precursor (Boc-Boc-Nos, 18.5
± 1.5 mg) dissolved in Acetonitrile (1.0 mL) is added to the reaction vessel. The reaction is heated at 135°C for 3 min. Radio-TLC indicated that the percent conversion of 18 F- fluoride to 18 F-Di-Boc FLT was >90% (Figure 4). The MeCN was removed under reduced pressure and heat. The crude material was subjected to deprotection conditions (HC1, IN, 105°C for 5 min). HPLC analytical analysis (10% EtOH:water) reveals the presence of 18 F-FLT with a purity of greater than 96% (Figure 5).
[0045] Synthesis of 18 F-HX4 acetate and "F-HX4 (Entries 6 and 7 :
Acetate b) 1 M K 2 C0 3 , 100°C, 300 sec
HX-4
[0046] [ ,8 F]-3-Fluoro-2-(4-((2-riitro-lH-in^^
yl)propan-l-ol ("HX4" of " ,8 F-HX4") precursor (18.5 ± 1.5 mg) dissolved in
Acetonitrile (1.0 mL) is added to the reaction vessel. The reaction is heated at 110°C for 10 min. Radio-TLC indicated that the percent conversion of 18 F- fluoride to 18 F-HX4 and 1 8 F-HX4 acetate was >90% (Figure 6). In a second run, the reaction was repeated and the labeling efficiency was monitored by RadioHPLC. After the fluorination step, >90% of the 18 F-fluoride was converted into the labeled intermediate ,8 F-HX4-OAc (Figure 7). The MeCN was removed under reduced pressure and heat. The mixture was further heated with K 2 C0 3 (1M) at lOOC for 300 seconds to complete the deprotection step. The conversion of 18 F-HX4-OAc into 18 F-HX4 was determined to be greater than 70% by radioHPLC (Figure 8).
[0047] While this invention has . been described in conjunction with the specific
embodiments outlined above, it is evident that many alternatives, modifications, and variations will be apparent to those skilled in the art. Accordingly, the preferred embodiments of the invention as set forth above are intended to be illustrative, not limiting. A variety of modifications to the embodiments described will be apparent to those skilled in the art from the disclosure provided herein. Thus, the present invention may be embodied in other specific forms without departing from the spirit or essential attributes thereof. Various changes may be made without departing from the spirit and scope of the inventions as defined in the following claims.