Sun J, Qian Y, Hamilton A D, Sebti S M
Department of Pharmacology, School of Medicine, University of Pittsburgh, Pennsylvania 15261, USA.
Cancer Res. 1995 Oct 1;55(19):4243-7.
Farnesylation of the oncoprotein Ras is required for its cancer-causing activity. We have designed farnesyltransferase inhibitor (FTI)-276, a tetrapeptide mimetic of the carboxyl terminus of K-Ras4B, as a highly potent and selective inhibitor of Ras farnesylation in vitro and in vivo. FTI-276 blocked the growth in nude mice of a human lung carcinoma that expresses the two most prevalent genetic alterations in human cancers (K-Ras oncogenic mutation and deletion in the tumor suppressor gene p53). In contrast, FTI-276 did not inhibit tumor growth of a human lung carcinoma that harbors no Ras mutations. Furthermore, FTI-276 inhibited oncogenic signaling and tumor growth of NIH 3T3 cells transformed with the ras but not the raf oncogene. Inhibition of tumor growth in vivo was dose dependent and correlated with inhibition of Ras processing in tumors in vivo. The work described here identifies FTI-276 as a highly selective suppressor of Ras-dependent oncogenicity and suggests that a broad spectrum of human cancers with aberrant Ras function could benefit from farnesyltransferase inhibitor treatment.
癌蛋白Ras的法尼基化是其致癌活性所必需的。我们设计了法尼基转移酶抑制剂(FTI)-276,它是K-Ras4B羧基末端的四肽模拟物,在体外和体内都是Ras法尼基化的高效选择性抑制剂。FTI-276抑制了一种人类肺癌在裸鼠中的生长,该肺癌表达了人类癌症中两种最常见的基因改变(K-Ras致癌突变和肿瘤抑制基因p53缺失)。相比之下,FTI-276不抑制无Ras突变的人类肺癌的肿瘤生长。此外,FTI-276抑制了用ras而非raf癌基因转化的NIH 3T3细胞的致癌信号传导和肿瘤生长。体内肿瘤生长的抑制是剂量依赖性的,并且与体内肿瘤中Ras加工的抑制相关。本文所述工作将FTI-276鉴定为Ras依赖性致癌性的高度选择性抑制剂,并表明广泛的具有异常Ras功能的人类癌症可能从法尼基转移酶抑制剂治疗中受益。
