eIF4A标准
翻译(生物学)
EIF4A1
解旋酶
生物
基因亚型
真核翻译
计算生物学
起始因子
真核起始因子
EIF4E公司
RNA解旋酶A
基因
信使核糖核酸
遗传学
核糖核酸
作者
Farheen Raza,Joseph A. Waldron,John Le Quesne
摘要
The malignant phenotype is largely the consequence of dysregulated gene expression. Transformed cells depend upon not just a global increase in protein synthesis but an altered translational landscape in which pro-oncogenic mRNAs are translationally up-regulated. Such mRNAs have been shown to possess longer and more structured 5′-UTRs requiring high levels of eukaryotic initiation factor 4A (eIF4A) helicase activity for efficient translation. As such there is a developing focus on targeting eIF4A as a cancer therapy. In order for such treatments to be successful, we must develop a detailed understanding of the mechanisms which make specific mRNAs more dependent on eIF4A activity than others. It is also crucial to fully characterize the potentially distinct roles of eIF4A1 and eIF4A2, which until recently were thought to be functionally interchangeable. This review will highlight the recent advances made in this field that address these issues.
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