Integrating amino acids into Bcr-Abl inhibitors: design, synthesis, biological evaluation, and in silico studies†

IF 3.597 Q2 Pharmacology, Toxicology and Pharmaceutics
MedChemComm Pub Date : 2024-07-24 DOI:10.1039/D4MD00417E
Yuying Liu, Zeyu Yang, Jie Zhang, Na Guo, Nanxin Liu, Qingqing Zhang, Xintao Dang, Yanchen Li, Jie Zhang and Xiaoyan Pan
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引用次数: 0

Abstract

Bcr-Abl is successfully applied to drug discovery as a CML therapeutic target, but point mutation resistance has become a major challenge in the clinical treatment of CML. Our previous studies have shown that the introduction of amino acids as flexible linkers and heterocyclic structures as HBMs can achieve potent inhibition of Bcr-AblT315I. In continuation of these studies, we further enriched the linker types by developing a library of compounds with tert-leucine or serine as a linker. Biological results showed that these compounds exhibited enhanced inhibition against Bcr-AblWT and Bcr-AblT315I kinases as well as improved antiproliferative activity in leukemia cell assays compared to previously disclosed compounds. In particular, compounds TL8, TL10, BS4, BS10, SR5 and SR11 exhibited potent inhibitory activities against Ba/F3 cells bearing a T315I mutant. Additionally, compounds TL8, BS4 and SR5 effectively induced K562 cell apoptosis, arrested the cell cycle at the S or G2/M phase, and inhibited the phosphorylation of Bcr-Abl and STAT5 in a dose-dependent manner. Docking studies verified the rationality of tert-leucine or serine as a flexible linker and indicated that phenylpyridine with an amide side chain favored the potency of these inhibitors. Moreover, ADME prediction suggested that the tested compounds had a favorable safety profile. Thus, tert-leucine or serine can be used as a promising class of flexible linkers for Bcr-Abl inhibitors with heterocyclic structures as HBMs, and compounds BS4, SR5, and especially TL8, can be used as starting points for further optimization.

Abstract Image

Abstract Image

将氨基酸整合到 Bcr-Abl 抑制剂中:设计、合成、生物评估和硅学研究。
Bcr-Abl作为CML治疗靶点已成功应用于药物研发,但点突变耐药已成为CML临床治疗的一大挑战。我们之前的研究表明,引入氨基酸作为柔性连接体和杂环结构作为 HBM 可以实现对 Bcr-AblT315I 的强效抑制。在这些研究的基础上,我们进一步丰富了连接体类型,开发了以叔亮氨酸或丝氨酸为连接体的化合物库。生物学结果表明,与之前公开的化合物相比,这些化合物对 Bcr-AblWT 和 Bcr-AblT315I 激酶的抑制作用增强,在白血病细胞实验中的抗增殖活性也有所提高。特别是,化合物 TL8、TL10、BS4、BS10、SR5 和 SR11 对带有 T315I 突变体的 Ba/F3 细胞具有强效抑制活性。此外,化合物 TL8、BS4 和 SR5 还能有效诱导 K562 细胞凋亡,使细胞周期停滞在 S 期或 G2/M 期,并以剂量依赖的方式抑制 Bcr-Abl 和 STAT5 的磷酸化。对接研究验证了叔亮氨酸或丝氨酸作为柔性连接体的合理性,并表明带有酰胺侧链的苯基吡啶更有利于提高这些抑制剂的效力。此外,ADME 预测表明,所测试的化合物具有良好的安全性。因此,叔亮氨酸或丝氨酸可以作为一类很有前景的柔性连接物,用于具有杂环结构的 Bcr-Abl 抑制剂 HBM,化合物 BS4、SR5,尤其是 TL8 可以作为进一步优化的起点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
MedChemComm
MedChemComm BIOCHEMISTRY & MOLECULAR BIOLOGY-CHEMISTRY, MEDICINAL
CiteScore
4.70
自引率
0.00%
发文量
0
审稿时长
2.2 months
期刊介绍: Research and review articles in medicinal chemistry and related drug discovery science; the official journal of the European Federation for Medicinal Chemistry. In 2020, MedChemComm will change its name to RSC Medicinal Chemistry. Issue 12, 2019 will be the last issue as MedChemComm.
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