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Design and Synthesis of IsoquinolidinobenzodiazepineDimers a Novel Class of Antibody–Drug Conjugate Payload

机译:异喹啉基苯并二氮杂pine的设计与合成Dimers一类新型的抗体-药物结合有效载荷

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摘要

Antibody–drug conjugates (ADCs) represent an important class of emerging cancer therapeutics. Recent ADC development efforts highlighted the use of pyrrolobenzodiazepine (PBD) dimer payload for the treatment of several cancers. We identified the isoquinolidinobenzodiazepine (IQB) payload (D211), a new class of PBD dimer family of DNA damaging payloads. We have successfully synthesized all three IQB stereoisomers, experimentally showed that the purified (S,S)-D211 isomer is functionally more active than (R,R)-D221 and (S,R)-D231 isomers by >50,000-fold and ∼200-fold, respectively. We also synthesized a linker-payload (D212) that uses (S,S)-D211 payload with a cathepsin cleavable linker, a hydrophilic PEG8 spacer, and a thiol reactive maleimide. In addition, homogeneous ADCs generated using D212 linker-payload exhibited ideal physicochemical properties, and anti-CD33 ADC displayed a robust target-specific potency on AML cell lines. These results demonstrate that D212 linker-payload described here can be utilized for developing novel ADC therapeutics for targeted cancer therapy.
机译:抗体-药物偶联物(ADC)代表了新兴的癌症治疗剂的重要类别。 ADC的最新开发成果强调了吡咯并苯并二氮杂(PBD)二聚体有效载荷在多种癌症治疗中的应用。我们确定了异喹啉苯并二氮杂卓(IQB)有效载荷(D211),这是一类新的PBD二聚体家族,可破坏DNA。我们已经成功合成了所有三种IQB立体异构体,实验表明纯化的(S,S)-D211异构体在功能上比(R,R)-D221和(S,R)-D231异构体活性高50,000倍以上〜分别为200倍。我们还合成了使用(S,S)-D211有效负载与组织蛋白酶可裂解的连接基,亲水性PEG8间隔基和硫醇反应性马来酰亚胺的连接基有效载荷(D212)。此外,使用D212接头有效负载生成的同质ADC表现出理想的理化性质,而抗CD33 ADC在AML细胞系上显示出强大的靶标特异性效能。这些结果表明,本文所述的D212接头有效负载可用于开发新型ADC治疗剂,用于靶向癌症治疗。

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