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首页> 外文期刊>Journal of Medicinal Chemistry >Antibody-Mediated Delivery of Chimeric BRD4 Degraders. Part 1: Exploration of Antibody Linker, Payload Loading, and Payload Molecular Properties
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Antibody-Mediated Delivery of Chimeric BRD4 Degraders. Part 1: Exploration of Antibody Linker, Payload Loading, and Payload Molecular Properties

机译:抗体介导的嵌合BRD4降解剂的递送。 第1部分:抗体接头探索,有效载荷和有效载荷分子特性

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摘要

The biological and medicinal impacts of proteolysis-targeting chimeras (PROTACs) and related chimeric molecules that effect intracellular degradation of target proteins via ubiquitin ligase-mediated ubiquitination continue to grow. However, these chimeric entities are relatively large compounds that often possess molecular characteristics, which may compromise oral bioavailability, solubility, and/or in vivo pharmacokinetic properties. We therefore explored the conjugation of such molecules to monoclonal antibodies using technologies originally developed for cytotoxic payloads so as to provide alternate delivery options for these novel agents. In this report, we describe the first phase of our systematic development of antibody-drug conjugates (ADCs) derived from bromodomain-containing protein 4 (BRD4)-targeting chimeric degrader entities. We demonstrate the antigendependent delivery of the degrader payloads to PC3-S1 prostate cancer cells along with related impacts on MYC transcription and intracellular BRD4 levels. These experiments culminate with the identification of one degrader conjugate, which exhibits antigendependent antiproliferation effects in LNCaP prostate cancer cells.
机译:蛋白质水解靶向嵌合体(PROTACs)和通过泛素连接酶介导的泛素化作用影响靶蛋白细胞内降解的相关嵌合体分子的生物学和医学影响继续增长。然而,这些嵌合体是相对较大的化合物,通常具有分子特征,这可能会影响口服生物利用度、溶解度和/或体内药代动力学特性。因此,我们利用最初为细胞毒性有效载荷开发的技术,探索了此类分子与单克隆抗体的结合,以便为这些新型药物提供替代递送选择。在本报告中,我们描述了我们系统开发的抗体-药物结合物(ADC)的第一阶段,ADC来源于含溴多巴胺的蛋白质4(BRD4)靶向嵌合降解物实体。我们证明了降解物有效载荷对PC3-S1前列腺癌细胞的抗依赖性传递,以及对MYC转录和细胞内BRD4水平的相关影响。这些实验最终确定了一种降解物结合物,该结合物在LNCaP前列腺癌细胞中表现出抗依赖性抗增殖作用。

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