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Ras Isoforms from Lab Benches to Lives—What Are We Missing and How Far Are We?

机译:来自实验室长椅的Ras Isoforms - 我们错过了什么我们有多远?

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摘要

The central protein in the oncogenic circuitry is the Ras GTPase that has been under intense scrutiny for the last four decades. From its discovery as a viral oncogene and its non-oncogenic contribution to crucial cellular functioning, an elaborate genetic, structural, and functional map of Ras is being created for its therapeutic targeting. Despite decades of research, there still exist lacunae in our understanding of Ras. The complexity of the Ras functioning is further exemplified by the fact that the three canonical Ras genes encode for four protein isoforms (H-Ras, K-Ras4A, K-Ras4B, and N-Ras). Contrary to the initial assessment that the H-, K-, and N-Ras isoforms are functionally similar, emerging data are uncovering crucial differences between them. These Ras isoforms exhibit not only cell-type and context-dependent functions but also activator and effector specificities on activation by the same receptor. Preferential localization of H-, K-, and N-Ras in different microdomains of the plasma membrane and cellular organelles like Golgi, endoplasmic reticulum, mitochondria, and endosome adds a new dimension to isoform-specific signaling and diverse functions. Herein, we review isoform-specific properties of Ras GTPase and highlight the importance of considering these towards generating effective isoform-specific therapies in the future.
机译:致癌电路中的中枢蛋白是过去四十年的强烈审查的RAS GTP酶。从其发现作为病毒性癌基因及其非致癌贡献,对关键的细胞功能,旨在为其治疗靶向产生RA的精细遗传,结构和功能图。尽管有数十年的研究,但我们对RAS的理解仍然存在。 RAS功能的复杂性进一步举例说明了三种规范RA基因编码四种蛋白质同种型(H-RAS,K-RAS4A,K-RAS4B和N-RAS)。与初始评估相反,H-,K-和N-RAS同种型在功能上相似,新兴数据正在揭示它们之间的至关重要差异。这些Ras同种型不仅表现出细胞型和上下文依赖性功能,而且表现出同一受体激活的活化剂和效应特异性。在血浆膜和细胞细胞细胞的不同微粒子中优先定位H-,K-和N-Ras,如Golgi,内质网,线粒体和内体为同种型信号传导和不同功能增加了新的尺寸。在此,我们回顾了RAS GTP酶的同种型特性,并突出了将来考虑到产生有效的同种类特异性疗法的重要性。

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