首页> 外文期刊>Journal of Medicinal Chemistry >Antibody-Mediated Delivery of Chimeric BRD4 Degraders. Part 2: Improvement of In Vitro Antiproliferation Activity and In Vivo Antitumor Efficacy
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Antibody-Mediated Delivery of Chimeric BRD4 Degraders. Part 2: Improvement of In Vitro Antiproliferation Activity and In Vivo Antitumor Efficacy

机译:抗体介导的嵌合BRD4降解剂的递送。 第2部分:改善体外抗溶解活性和体内抗肿瘤效力

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摘要

Heterobifunctional compounds that direct the ubiquitination of intracellular proteins in a targeted manner via coopted ubiquitin ligases have enormous potential to transform the field of medicinal chemistry. These chimeric molecules, often termed proteolysis-targeting chimeras (PROTACs) in the chemical literature, enable the controlled degradation of specific proteins via their direction to the cellular proteasome. In this report, we describe the second phase of our research focused on exploring antibody-drug conjugates (ADCs), which incorporate BRD4-targeting chimeric degrader entities. We employ a new BRD4-binding fragment in the construction of the chimeric ADC payloads that is significantly more potent than the corresponding entity utilized in our initial studies. The resulting BRD4-degrader antibody conjugates exhibit potent and antigen-dependent BRD4 degradation and antiproliferation activities in cell-based experiments. Multiple ADCs bearing chimeric BRD4-degrader payloads also exhibit strong, antigen-dependent antitumor efficacy in mouse xenograft assessments that employ several different tumor models.
机译:通过结合泛素连接酶以靶向方式指导细胞内蛋白质泛素化的异源双功能化合物具有巨大的潜力,可以改变药物化学领域。这些嵌合体分子,在化学文献中通常被称为蛋白质水解靶向嵌合体(PROTACs),能够通过其指向细胞蛋白酶体的方向来控制特定蛋白质的降解。在本报告中,我们描述了我们研究的第二阶段,重点是探索抗体-药物结合物(ADC),它结合BRD4靶向嵌合降解物实体。我们在构建嵌合ADC有效载荷时使用了一个新的BRD4结合片段,该片段的效力明显高于我们最初研究中使用的相应实体。由此产生的BRD4降解物抗体结合物在基于细胞的实验中表现出有效的和抗原依赖性的BRD4降解和抗增殖活性。在采用几种不同肿瘤模型的小鼠异种移植评估中,携带嵌合BRD4降解物有效载荷的多个ADC也表现出强大的抗原依赖性抗肿瘤功效。

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