Kohl N E, Wilson F R, Mosser S D, Giuliani E, deSolms S J, Conner M W, Anthony N J, Holtz W J, Gomez R P, Lee T J
Department of Cancer Research, Merck Research Laboratories, West Point, PA 19486.
Proc Natl Acad Sci U S A. 1994 Sep 13;91(19):9141-5. doi: 10.1073/pnas.91.19.9141.
The posttranslational addition of a farnesyl moiety to the Ras oncoprotein is essential for its transforming activity. Cell-active inhibitors of the enzyme that catalyzes this reaction, protein farnesyltransferase, have been shown to selectively block ras-dependent transformation of cells in culture. Here we describe the protein farnesyltransferase inhibitor 2(S)-[2(S)-[2(R)-amino-3-mercapto]propylamino-3(S)-methyl] pentyloxy-3-phenylpropionylmethioninesulfone methyl ester (L-739,749), which suppressed the anchorage-independent growth of Rat1 cells transformed with viral H-ras and the human pancreatic adenocarcinoma cell line PSN-1, which harbors altered K-ras, myc, and p53 genes. This compound also suppressed the growth of tumors arising from ras-transformed Rat1 cells in nude mice by 66%. Under the same conditions, doxorubicin inhibited tumor growth by 33%. Control tumors formed by v-raf- or v-mos-transformed Rat1 cells were unaffected by L-739,749. Furthermore, mice treated with L-739,749 exhibited no evidence of systemic toxicity. This is a demonstration of antitumor activity in vivo using a synthetic small molecule inhibitor of protein farnesyltransferase.
将法尼基部分翻译后添加到Ras癌蛋白上对其转化活性至关重要。催化此反应的酶(蛋白法尼基转移酶)的细胞活性抑制剂已被证明能在培养中选择性阻断细胞的ras依赖性转化。在此我们描述蛋白法尼基转移酶抑制剂2(S)-[2(S)-[2(R)-氨基-3-巯基]丙基氨基-3(S)-甲基]戊氧基-3-苯基丙酰甲硫氨酸砜甲酯(L-739,749),它抑制了用病毒H-ras转化的Rat1细胞以及携带改变的K-ras、myc和p53基因的人胰腺腺癌细胞系PSN-1的不依赖贴壁生长。该化合物还使裸鼠中由ras转化的Rat1细胞产生的肿瘤生长抑制了66%。在相同条件下,阿霉素抑制肿瘤生长33%。由v-raf或v-mos转化的Rat1细胞形成的对照肿瘤不受L-739,749影响。此外,用L-739,749处理的小鼠未表现出全身毒性的迹象。这是使用蛋白法尼基转移酶的合成小分子抑制剂在体内抗肿瘤活性的一个例证。
