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Identification of Novel Fused Heteroaromatics-Based MALT1 Inhibitors by High-Throughput Screening to Treat B Cell Lymphoma

机译:通过高通量筛选鉴定基于融合杂芳烃的新型 MALT1 抑制剂治疗 B 细胞淋巴瘤

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摘要

Development of mucosa-associated lymphoid tissue lymphoma translocation protein 1 (MALT1) inhibitors is of great value and significance in the treatment of neoplastic disorders and inflammatory and autoimmune diseases. However, there is a lack of effective MALT1 inhibitors in clinic. Herein, a novel class of potent 5-oxo-1-thioxo-4,5-dihydro-1H-thiazolo3,4-aquinazoline-based MALT1 inhibitors and their covalent derivatives were first identified and designed through high-throughput screening. We demonstrated that compounds 15c, 15e, and 20c effectively inhibited the MALT1 protease and displayed selective cytotoxicity to activated B cell-like diffuse large B cell lymphoma with low single-digit micromolar potency. Furthermore, compound 20c specifically repressed NF-.B signaling and induced cell apoptosis in MALT1-dependent TMD8 cells in a dose-dependent manner. More importantly, 20c showed good pharmacokinetic properties and antitumor efficacy with no significant toxicity in the TMD8 xenograft tumor model. Collectively, this study provides valuable lead compounds of MALT1 inhibitors for further structural optimization and antitumor mechanism study.
机译:黏膜相关淋巴组织易位蛋白1(MALT1)抑制剂的开发在肿瘤性疾病、炎症性和自身免疫性疾病的治疗中具有重要价值和意义。然而,临床上缺乏有效的 MALT1 抑制剂。本文首先通过高通量筛选鉴定和设计了一类新型的强效5-氧代-1-硫代-4,5-二氢-1H-噻唑并[3,4-a]喹唑啉类MALT1抑制剂及其共价衍生物。我们证明化合物 15c、15e 和 20c 有效抑制 MALT1 蛋白酶,并对活化的 B 细胞样弥漫性大 B 细胞淋巴瘤表现出选择性细胞毒性,效力低个位数微摩尔效力。此外,化合物20c特异性地抑制了NF-。以剂量依赖性方式在 MALT1 依赖性 TMD8 细胞中诱导 B 信号转导和诱导细胞凋亡。更重要的是,20c在TMD8异种移植肿瘤模型中显示出良好的药代动力学特性和抗肿瘤功效,无显著毒性。本研究为进一步的结构优化和抗肿瘤机制研究提供了有价值的MALT1抑制剂先导化合物。

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