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Cell death-independent activities of the death receptors CD95, TRAILR1, and TRAILR2

机译:Cell Death-Death-Death受体的活动活动CD95,Trailr1和Trailr2

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摘要

Since their identification more than 20 years ago, the death receptors CD95, TRAILR1, and TRAILR2 have been intensively studied with respect to their cell death-inducing activities. These receptors, however, can also trigger a variety of cell death-independent cellular responses reaching from the activation of proinflammatory gene transcription programs over the stimulation of proliferation and differentiation to induction of cell migration. The cell death-inducing signaling mechanisms of CD95 and the TRAIL death receptors are well understood. In contrast, despite the increasing recognition of the biological and pathophysiological relevance of the cell death-independent activities of CD95, TRAILR1, and TRAILR2, the corresponding signaling mechanisms are less understood and give no fully coherent picture. This review is focused on the cell death-independent activities of CD95 and the TRAIL death receptors and addresses mainly three questions: (a) how are these receptors linked to noncell death pathways at the molecular level, (b) which factors determine the balance of cell death and cell death-independent activities of CD95 and the TRAIL death receptors at the cellular level, and (c) what are the consequences of the cell death-independent functions of these receptors for their role in cancer and inflammatory diseases.
机译:由于他们的识别超过20年前,死亡受体CD95,TrailR1和Trantr2已经广泛研究了他们的细胞死亡诱导的活动。然而,这些受体还可以引发各种细胞死亡的细胞反应,从促炎基因转录方案的激活达到促进细胞迁移的诱导和分化的激活。 CD95和TRAIL死亡受体的细胞死亡信令机制很好地理解。相反,尽管对CD95,铁路1和滑轨2的细胞死亡活动的生物学和病理生理学相关性的识别不断升高,但相应的信令机制较少理解并没有完全相干的图像。本综述专注于CD95和TRAIL死亡受体的细胞死亡活动,以及地址主要是三个问题:(a)这些受体如何与分子水平的非细胞死亡途径相关联(b)哪些因素决定了余额CD95的细胞死亡和细胞死亡活动和细胞水平的痕量死亡受体,(c)这些受体对癌症和炎症性疾病中作用的细胞死亡职能的后果是什么。

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