通过伊马替尼衍生物与cIAP1配体的共轭作用开发BCR-ABL降解诱导剂。

Development of BCR-ABL degradation inducers via the conjugation of an imatinib derivative and a cIAP1 ligand.

作者信息

Demizu Yosuke, Shibata Norihito, Hattori Takayuki, Ohoka Nobumichi, Motoi Hiromi, Misawa Takashi, Shoda Takuji, Naito Mikihiko, Kurihara Masaaki

机构信息

Division of Organic Chemistry, National Institute of Health Sciences, Tokyo, Japan.

Division of Molecular Target and Gene Therapy Products, National Institute of Health Sciences, Tokyo, Japan.

出版信息

Bioorg Med Chem Lett. 2016 Oct 15;26(20):4865-4869. doi: 10.1016/j.bmcl.2016.09.041. Epub 2016 Sep 15.

DOI:10.1016/j.bmcl.2016.09.041

PMID:27666635

Abstract

The manipulation of protein stability with small molecules has great potential as a technique for aiding the development of clinical therapies, including treatments for cancer. In this study, BCR-ABL protein degradation inducers called SNIPER(ABL) (Specific and Non-genetic inhibitors of apoptosis protein [IAP]-dependent Protein Erasers) were developed. The designed molecules contained two biologically active scaffolds: one was an imatinib derivative that binds to BCL-ABL and the other was a methyl bestatin that binds to cellular IAP 1 (cIAP1). The hybrid molecules, SNIPER(ABL), were expected to recruit BCR-ABL to cIAP1 for removal by proteasomes. In fact, SNIPER(ABL) induced the degradation of BCR-ABL protein and a subsequent reduction in cell growth. Thus, the degradation of BCR-ABL by SNIPER(ABL) is one potential strategy for treating BCR-ABL driven chronic myelogenous leukemia.

摘要

利用小分子调控蛋白质稳定性作为一种辅助临床治疗方法（包括癌症治疗）的技术具有巨大潜力。在本研究中，开发了一种名为SNIPER(ABL)（凋亡蛋白[IAP]依赖性蛋白清除剂的特异性非遗传抑制剂）的BCR-ABL蛋白降解诱导剂。设计的分子包含两个生物活性支架：一个是与BCL-ABL结合的伊马替尼衍生物，另一个是与细胞IAP 1（cIAP1）结合的甲基苯丁抑制素。杂合分子SNIPER(ABL)有望将BCR-ABL募集到cIAP1以被蛋白酶体清除。事实上，SNIPER(ABL)诱导了BCR-ABL蛋白的降解以及随后细胞生长的减少。因此，SNIPER(ABL)介导的BCR-ABL降解是治疗BCR-ABL驱动的慢性粒细胞白血病的一种潜在策略。

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通过伊马替尼衍生物与cIAP1配体的共轭作用开发BCR-ABL降解诱导剂。

Development of BCR-ABL degradation inducers via the conjugation of an imatinib derivative and a cIAP1 ligand.

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