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通过连接子稳定化和与转甲状腺素蛋白结合配体缀合来提高基于 PSMA 的小分子药物偶联物的安全性和疗效。

Enhancing the Safety and Efficacy of PSMA-Based Small-Molecule Drug Conjugates by Linker Stabilization and Conjugation to Transthyretin Binding Ligand.

机构信息

Department of Pharmaceutics and Medicinal Chemistry, Thomas J. Long School of Pharmacy, University of the Pacific, Stockton, California 95211, United States.

出版信息

J Med Chem. 2022 Nov 24;65(22):15473-15486. doi: 10.1021/acs.jmedchem.2c01423. Epub 2022 Nov 3.

Abstract

This work describes the enhancement of a novel antitumor therapeutic platform that combines advantages from small-molecule drug conjugates (SMDCs) and antibody drug conjugates (ADCs). Valine-citrulline (VCit) dipeptide linkers are commonly used cathepsin B cleavable linkers for ADCs. However, the instability of these linkers in mouse serum makes translating efficacy data from mouse to human more challenging. Replacing the VCit linker with glutamic acid-valine-citrulline (EVCit) has been reported to enhance the stability of ADCs in mouse serum. However, the effect of EVCit linker on the stability of SMDCs has not been reported. Here, we report that incorporating the EVCit linker in prostate-specific membrane antigen-targeting SMDCs, equipped with the transthyretin ligand AG10, resulted in conjugates with lower toxicity, an extended half-life, and superior therapeutic efficacy to docetaxel in a xenograft mouse model of prostate cancer. This should make SMDCs' preclinical toxicity and efficacy data from mice more reliable for predicting human results.

摘要

这项工作描述了一种新型抗肿瘤治疗平台的增强,该平台结合了小分子药物偶联物 (SMDC) 和抗体药物偶联物 (ADC) 的优势。缬氨酸-瓜氨酸 (VCit) 二肽接头通常用于 ADC 的组织蛋白酶 B 可切割接头。然而,这些接头在小鼠血清中的不稳定性使得将疗效数据从小鼠转化为人类更具挑战性。据报道,用谷氨酸-缬氨酸-瓜氨酸 (EVCit) 取代 VCit 接头可以提高 ADC 在小鼠血清中的稳定性。然而,EVCit 接头对 SMDC 稳定性的影响尚未报道。在这里,我们报告说,在前列腺特异性膜抗原靶向 SMDC 中加入 EVCit 接头,并配备转甲状腺素蛋白配体 AG10,可导致与多西他赛相比,在前列腺癌异种移植小鼠模型中具有更低的毒性、更长的半衰期和更好的治疗效果。这应该使 SMDC 的临床前毒性和疗效数据从小鼠更可靠地预测人类的结果。

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