Mazières Julien, Pradines Anne, Favre Gilles
Inserm U.563, Centre de Physiopathologie Toulouse Purpan, Département Innovation Thérapeutique et Oncologie Moléculaire, Institut Claudius Regaud, 20-24, rue du pont Saint-Pierre, 31052 Toulouse, France.
Med Sci (Paris). 2003 Feb;19(2):211-6. doi: 10.1051/medsci/2003192211.
The fact that proteins such as Ras require farnesylation to induce malignant transformation prompted many investigators to design farnesyl transferase inhibitors (FTI) as novel anticancer drugs. FTIs inhibit the growth of ras transformed cells in vitro and induce tumor regression in ras dependent tumor in vivo. Moreover, FTIs inhibit tumor progression in human tumor xenograft models. Currently, FTIs are undergoing phase I and II trials in various cancer types. They show impressive antitumour efficacy and they lack toxicity. Despite these promising results, the development of such molecules in hindered by the absence of appropriate clinical endpoints and of surrogate biological markers. Indeed, it seems likely that Ras is not the critical target of FTIs and that inhibition of the farnesylation of proteins such as RhoB, might also contribute to the observed antitumour properties. Identification of targets that underlie their biological effect is essential in order to predict and evaluate their efficacy.
诸如Ras等蛋白质需要法尼基化才能诱导恶性转化,这一事实促使许多研究人员设计法尼基转移酶抑制剂(FTI)作为新型抗癌药物。FTI在体外抑制ras转化细胞的生长,并在体内诱导ras依赖性肿瘤的消退。此外,FTI在人肿瘤异种移植模型中抑制肿瘤进展。目前,FTI正在多种癌症类型中进行I期和II期试验。它们显示出令人印象深刻的抗肿瘤疗效且无毒性。尽管有这些令人鼓舞的结果,但由于缺乏合适的临床终点和替代生物标志物,此类分子的开发受到阻碍。事实上,Ras似乎不是FTI的关键靶点,抑制RhoB等蛋白质的法尼基化也可能有助于观察到的抗肿瘤特性。确定其生物学效应背后的靶点对于预测和评估其疗效至关重要。
