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Proapoptotic role of novel gene-expression factors

机译:新型基因表达因子的促凋亡作用

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摘要

The mechanisms that control cellular proliferation, as well as those related with programmed cell death or apopotosis, require precise regulation systems to prevent diseases such as cancer. Events related to cellular proliferation as well as those associated with apoptosis involve the regulation of gene expression carried out by three basic genetic expression regulation mechanisms: transcription, splicing of the primary transcript for mature mRNA formation, and RNA translation, a ribosomal machinery-dependent process for protein synthesis. While development of each one of these processes requires energy for recognition and assembly of a number of molecular complexes, it has been reported that an increased expression of several members of these protein complexes promotes apoptosis in distinct cell types. The question of how these factors interact with other proteins in order to incorporate themselves into the different transduction cascades and stimulate the development of programmed cell death, although nowadays actively studied, is still waiting for a clear-cut answer. This review focuses on the interactions established between different families of transcription, elongation, translation and splicing factors associated to the progression of apoptosis.
机译:控制细胞增殖的机制以及与程序性细胞死亡或细胞凋亡相关的机制,需要精确的调控系统来预防癌症等疾病。与细胞增殖相关的事件以及与凋亡相关的事件涉及通过三种基本的基因表达调控机制进行的基因表达调控:转录,成熟的mRNA形成的主要转录物的剪接和RNA的翻译(依赖核糖体机制的过程)用于蛋白质合成。虽然开发这些过程中的每一个都需要能量来识别和组装许多分子复合物,但是据报道,这些蛋白质复合物的几种成员表达的增加促进了不同细胞类型的凋亡。这些因素如何与其他蛋白质相互作用,以使其自身整合到不同的转导级联反应中,并刺激程序性细胞死亡的发展,这一问题尽管正在积极研究中,但仍在等待一个明确的答案。这篇综述着重于与凋亡进程相关的转录,延伸,翻译和剪接因子的不同家族之间建立的相互作用。

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