靶向 mRNA 翻译的新兴治疗方法。
Emerging therapeutics targeting mRNA translation.
机构信息
Department of Biochemistry and McGill University, Montréal, Québec H3G 1Y6, Canada.
出版信息
Cold Spring Harb Perspect Biol. 2012 Apr 1;4(4):a012377. doi: 10.1101/cshperspect.a012377.
Abstract
A defining feature of many cancers is deregulated translational control. Typically, this occurs at the level of recruitment of the 40S ribosomes to the 5'-cap of cellular messenger RNAs (mRNAs), the rate-limiting step of protein synthesis, which is controlled by the heterotrimeric eukaryotic initiation complex eIF4F. Thus, eIF4F in particular, and translation initiation in general, represent an exploitable vulnerability and unique opportunity for therapeutic intervention in many transformed cells. In this article, we discuss the development, mode of action and biological activity of a number of small-molecule inhibitors that interrupt PI3K/mTOR signaling control of eIF4F assembly, as well as compounds that more directly block eIF4F activity.
摘要
许多癌症的一个显著特征是翻译调控失控。通常,这种情况发生在 40S 核糖体与细胞信使 RNA(mRNA)5'-帽结合的水平上,这是蛋白质合成的限速步骤,由异三聚体真核起始复合物 eIF4F 控制。因此,eIF4F 特别是翻译起始,代表了许多转化细胞中可利用的脆弱性和独特的治疗干预机会。在本文中,我们讨论了一些小分子抑制剂的开发、作用模式和生物学活性,这些抑制剂可以阻断 PI3K/mTOR 信号通路对 eIF4F 组装的控制,以及一些更直接阻断 eIF4F 活性的化合物。
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