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Discovery of an Orally Efficacious MYC Inhibitor for Liver Cancer Using a GNMT-Based High-Throughput Screening System and Structure-Activity Relationship Analysis

机译:基于GNMT的高通量筛选系统发现一种口服有效的肝癌MYC抑制剂及构效关系分析

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Glycine-N-methyl transferase (GNMT) downregulation results in spontaneous hepatocellular carcinoma (HCC). Overexpression of GNMT inhibits the proliferation of liver cancer cell lines and prevents carcinogen-induced HCC, suggesting that GNMT induction is a potential approach for anti-HCC therapy. Herein, we used Huh7 GNMT promoter-driven screening to identify a GNMT inducer. Compound K78 was identified and validated for its induction of GNMT and inhibition of Huh7 cell growth. Subsequently, we employed structure-activity relationship analysis and found a potent GNMT inducer, K117. K117 inhibited Huh7 cell growth in vitro and xenograft in vivo. Oral administration of a dosage of K117 at 10 mpk (milligrams per kilogram) can inhibit Huh7 xenograft in a manner equivalent to the effect of sorafenib at a dosage of 25 mpk. A mechanistic study revealed that K117 is an MYC inhibitor. Ectopic expression of MYC using CMV promoter blocked K117-mediated MYC inhibition and GNMT induction. Overall, K117 is a potential lead compound for HCC- and MYC-dependent cancers.
机译:甘氨酸-N-甲基转移酶 (GNMT) 下调导致自发性肝细胞癌 (HCC)。GNMT的过表达抑制肝癌细胞系的增殖并防止致癌物诱导的HCC,表明GNMT诱导是抗HCC治疗的潜在方法。在此,我们使用 Huh7 GNMT 启动子驱动的筛选来鉴定 GNMT 诱导剂。鉴定并验证了化合物 K78 对 GNMT 的诱导和 Huh7 细胞生长的抑制作用。随后,我们采用构效关系分析,发现了一种有效的GNMT诱导剂K117。K117 在体外抑制 Huh7 细胞生长,在体内抑制异种移植。口服剂量为10mpk(毫克/千克)的K117可以抑制Huh7异种移植物,其方式相当于剂量为25mpk的索拉非尼的作用。一项机制研究表明,K117 是一种 MYC 抑制剂。使用 CMV 启动子阻断 K117 介导的 MYC 抑制和 GNMT 诱导的 MYC 异位表达。总体而言,K117是HCC和MYC依赖性癌症的潜在先导化合物。

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