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人类肿瘤中翻译失调的机制及治疗干预策略。

Mechanisms of translational deregulation in human tumors and therapeutic intervention strategies.

作者信息

Bilanges B, Stokoe D

机构信息

UCSF Cancer Research Institute, San Francisco, CA 94115, USA.

出版信息

Oncogene. 2007 Sep 6;26(41):5973-90. doi: 10.1038/sj.onc.1210431. Epub 2007 Apr 2.

Abstract

Analysis of the recurrent genetic aberrations present in human tumors provides insight into how normal cells escape appropriate proliferation and survival cues. Commonly mutated genes encode proteins that monitor DNA damage (e.g., p53), proteins that regulate the cell cycle (such as Rb), and proteins that regulate signal transduction pathways (such as APC, PTEN and Ras). Analysis of the relevant targets and downstream events of these genes in normal and tumor cells will clearly highlight important pathways for tumorigenesis. However, more infrequent mutations are also informative in defining events critical for the process of tumorigenesis, and often delineate important pathways lying downstream of commonly mutated oncogenes and tumor suppressors. Together, these studies have led to the conclusion that deregulated protein synthesis plays an important role in human cancer. This review will discuss the evidence implicating mRNA translation as an important downstream consequence of signal transduction pathways initiated by mutated oncogenes and tumor suppressors, as well as additional genetic findings implicating the importance of global and specific translational control in human cancer. It will also discuss therapeutic strategies that take advantage of differences in translational regulation between normal and tumor cells.

摘要

对人类肿瘤中存在的复发性基因畸变进行分析,有助于深入了解正常细胞如何逃避适当的增殖和生存信号。常见的突变基因编码监测DNA损伤的蛋白质(如p53)、调节细胞周期的蛋白质(如Rb)以及调节信号转导通路的蛋白质(如APC、PTEN和Ras)。对正常细胞和肿瘤细胞中这些基因的相关靶点及下游事件进行分析,将清晰地凸显肿瘤发生的重要通路。然而,较为罕见的突变在确定对肿瘤发生过程至关重要的事件方面也具有参考价值,并且常常勾勒出常见突变的癌基因和肿瘤抑制基因下游的重要通路。综合这些研究得出的结论是,蛋白质合成失调在人类癌症中起着重要作用。本综述将讨论相关证据,这些证据表明mRNA翻译是由突变的癌基因和肿瘤抑制基因引发的信号转导通路的重要下游结果,以及其他表明全局和特定翻译控制在人类癌症中的重要性的遗传学发现。还将讨论利用正常细胞和肿瘤细胞翻译调控差异的治疗策略。

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