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通过马来酰亚胺的 Diels-Alder 反应一步法生产抗体药物偶联物的反应性抗体平台。

A Reactive Antibody Platform for One-Step Production of Antibody-Drug Conjugates through a Diels-Alder Reaction with Maleimide.

机构信息

Department of Chemistry and Biochemistry , University of California , Santa Barbara , California 93106-9510 , United States.

Antibody Discovery and Protein Engineering Department , AstraZeneca R&D , Gaithersburg , Maryland 20878 , United States.

出版信息

Bioconjug Chem. 2019 Sep 18;30(9):2340-2348. doi: 10.1021/acs.bioconjchem.9b00436. Epub 2019 Aug 19.

Abstract

The normal electron-demand Diels-Alder (DA) cycloaddition is a classic transformation routinely used in synthesis; however, applications in biological systems are limited. Here, we report a spiro[2.4]hepta-4,6-diene-containing noncanonical amino acid (SCpHK) capable of efficient incorporation into antibodies and subsequent coupling with maleimide via a DA reaction. SCpHK was stable throughout protein expression in mammalian cells and enabled covalent attachment of maleimide drug-linkers yielding DA antibody-drug conjugates (DA-ADCs) with nearly quantitative conversion in a one-step process. The uncatalyzed DA reaction between SCpHK and maleimide in aqueous buffer was rapid (1.8-5.4 M s), and the antibody-drug adduct was stable in rat serum for at least 1 week at 37 °C. Anti-EphA2 DA-ADCs containing AZ1508 or SG3249 maleimide drug-linkers were potent inhibitors of tumor growth in PC3 tumor models in vivo. The DA bioconjugation strategy described here represents a simple method to produce site-specific and stable ADCs with maleimide drug-linkers.

摘要

正常的电子需求 Diels-Alder(DA)环加成是一种经典的合成转化,然而,在生物系统中的应用受到限制。在这里,我们报告了一种含有螺[2.4]庚-4,6-二烯的非典型氨基酸(SCpHK),能够有效地掺入抗体中,并通过 DA 反应与马来酰亚胺进行偶联。在哺乳动物细胞中表达蛋白质时,SCpHK 非常稳定,并能够通过 DA 反应将马来酰亚胺药物接头共价连接到抗体上,在一步法中几乎可以定量转化为 DA 抗体药物偶联物(DA-ADC)。在水性缓冲液中,SCpHK 和马来酰亚胺之间的非催化 DA 反应非常迅速(1.8-5.4 M s),抗体药物加合物在 37°C 的大鼠血清中至少稳定 1 周。含有 AZ1508 或 SG3249 马来酰亚胺药物接头的抗 EphA2 DA-ADC 在体内 PC3 肿瘤模型中具有很强的抑制肿瘤生长作用。这里描述的 DA 生物缀合策略代表了一种生产带有马来酰亚胺药物接头的定点和稳定 ADC 的简单方法。

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