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Preparation method of drug-linker MC-MMAF for antibody drug conjugate and intermediate thereof

A technology of intermediates and compounds, applied in the field of preparation of drug-linker MC-MMAF, can solve the problems of difficult post-processing and purification, affecting yield, increasing operating costs, etc. It is easier to control and reduce the difficulty of operation when reaching quality standards , Improve the effect of reactivity

Active Publication Date: 2019-06-25
LEVENA BIOPHARMA
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  • Summary
  • Abstract
  • Description
  • Claims
  • Application Information

AI Technical Summary

Problems solved by technology

[0010] There is a methyl group on the N of the N-terminal valine of this route MMAF, and the steric hindrance is relatively large. In this case, the reaction speed of connecting 1-maleimido n-hexanoic acid to MMAF will be slower. Racemization of the chiral carbon attached to the phenylpropanamide group of MMAF even with different amide condensing agents
This route is used for the synthesis of MC-MMAF less than 1g. Finally, high-pressure reverse phase preparation should be used to remove isomer impurities, and the yield is less than 50%.
[0011] This reaction route shows certain defects when enlarging production, such as: 1. This method causes 30-50% racemization because the condensing agent can activate the carboxyl group on MMAF simultaneously, forms the isomer impurity that is difficult to remove, affects Productivity; 2. Due to the aforementioned steric hindrance, the reaction time is long and there are many impurities, which cause difficulties in post-processing and purification of the reaction; 3. The final product needs high-pressure reverse-phase preparation to remove isomers, which increases operating costs; 4. Directly The toxin MMAF is used as a raw material, and a large number of synthetic operations need to be well protected, and the selection of protective equipment will bring obstacles to production operations

Method used

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  • Preparation method of drug-linker MC-MMAF for antibody drug conjugate and intermediate thereof
  • Preparation method of drug-linker MC-MMAF for antibody drug conjugate and intermediate thereof
  • Preparation method of drug-linker MC-MMAF for antibody drug conjugate and intermediate thereof

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Experimental program
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preparation example Construction

[0075] The invention provides a method for synthesizing MC-MMAF, the synthesis method comprising the steps of:

[0076] 1) Compound dissolved in a suitable solvent selected from dichloromethane, dimethylsulfoxide, N,N-dimethylformamide, N,N-dimethylacetamide, tetrahydrofuran, 1,4- One or more of dioxane and 2-methyltetrahydrofuran undergo amide condensation reaction with Val-Dil-Dap-Phe-OH to obtain MC-MMAF, and the structural formula of Val-Dil-Dap-Phe-OH is

[0077] In step 1), if R is hydrogen, reagent N is added under the action of reagent M selected from DCC, DCEP, EDC, DIC, HATU, HBTU, HBPIPU, HBPyU, HSPyU, HCTU, HOTU , HOTT, HSTU, HDMA, TATU, TBTU, TCTU, TCFH, TDBTU, TOTU, TOTT, TPTU, TFFH, BTFFH, TNTU, TSTU, COMU, T3P, BOP, PyBOP, PyBrOP, PyClOP, BrOP, PyAOP, PyCIU, CDI One or more of , TPSI, TSTU, DEPBT, DMTMM, EEDQ, CIP, CIB, DMC, HOBt and EDCI; more preferably, the reagent M is selected from one of EDCI, EDC, DIC, HOAt and HOBt More preferably, the reagent M i...

Embodiment 1

[0083] The reaction scheme of the present embodiment is as follows:

[0084]

[0085] Compound A1 (2.65g, 10.0mmol), HATU (4.56g, 12.0mmol) and DIEA (3.87g, 30.0mmol) were added to dichloromethane (50mL), stirred at room temperature for 30 minutes under nitrogen protection, and compound A2 was added (2.09g, 10.0mmol), stirring at room temperature under nitrogen protection for 4 hours, LCMS showed that the compound A1 in the reaction solution was less than 3%, and the reaction was considered complete. The reaction solution was washed successively with aqueous citric acid (20 mL), saturated brine (20 mL), dried over anhydrous sodium sulfate, and spin-dried. The crude product was slurried with a mixed solvent of 20 mL (petroleum ether: ethyl acetate = 10:1), filtered, and The obtained solid was washed with petroleum ether (10 mL) and sucked dry to obtain compound A3 (white solid, 3.92 g, yield 93%). MS: 421.16 (M+H + )

[0086] In a 100mL single-necked bottle, add 50mL of m...

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Abstract

The invention provides a preparation method of a drug-linker MC-MMAF for antibody coupling drugs and an intermediate thereof. According to the preparation method of the drug-linker MC-MMAF, the reaction activity of the N end is improved, the occurrence of racemization reaction is effectively controlled; toxin MMAF is not directly used, a fragment peptide with lower toxicity is adopted, the operation difficulty in mass production is reduced, no reverse phase preparation is needed, and the operation is simple and convenient.

Description

technical field [0001] The invention relates to the field of organic synthesis, in particular to a method for preparing drug-linker MC-MMAF used in antibody-drug conjugates and an intermediate thereof. Background technique [0002] Antibody drug conjugate (ADC) is a new type of anti-tumor drug. Its principle is to link cytotoxins to antibodies, recognize specific antigens on the surface of cancer cells through antibodies, and enter cancer cells through endocytosis. Cells, so as to transport cytotoxins to the target, to achieve the purpose of targeted treatment of malignant tumors. Compared with traditional small-molecule anti-tumor drugs, ADC is more specific and effective because it can rely on the target recognition of antibodies and the high activity of toxins. [0003] ADCs consist of three distinct components, namely antibodies, linkers and cytotoxins. The antibody achieves targeting, and the linker ensures the stability of the ADC during blood transport, and after re...

Claims

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Application Information

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IPC IPC(8): C07D207/452C07K5/027C07K1/02
CPCC07D207/452C07K1/02
Inventor 许喆李海泓郭茂君李辉
Owner LEVENA BIOPHARMA
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