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理解神经营养素的作用:最新进展与挑战。

Understanding proneurotrophin actions: Recent advances and challenges.

机构信息

Department of Medicine, Weill Cornell Medical College, New York, New York 10065, USA.

出版信息

Dev Neurobiol. 2010 Apr;70(5):350-9. doi: 10.1002/dneu.20768.

Abstract

Neurotrophins are initially synthesized as larger precursors (proneurotrophins), which undergo proteolytic cleavage to yield mature forms. Although the functions of the mature neurotrophins have been well established during neural development and in the adult nervous system, roles for the proneurotrophins in developmental and injury-induced cell death, as well as in synaptic plasticity, have only recently been appreciated. Interestingly, both mature neurotrophins and proneurotrophins utilize dual-receptor complexes to mediate their actions. The mature neurotrophin coreceptors consist of the Trk receptor tyrosine kinases and p75(NTR), wherein Trk transduces survival and differentiative signaling, and p75(NTR) modulates the affinity and selectivity of Trk activation. On the other hand, proneurotrophins engage p75(NTR) and the structurally distinct coreceptor sortilin, to initiate p75(NTR)-dependent signal transduction cascade. Although the specificity of mature neurotrophins vs. proneurotrophins actions is due in part to the formation of distinct coreceptor complexes, a number of recent studies highlight how different p75(NTR)-mediated cellular actions are modulated. Here, we review emerging evidence for a novel transmembrane mechanism for ligand-specific p75(NTR) activation and several mechanisms by which p75(NTR)-dependent apoptotic and nonapoptotic responses can be selective activated.

摘要

神经递生素最初被合成为较大的前体(前神经递生素),它们经过蛋白水解切割产生成熟形式。尽管成熟的神经递生素在神经发育和成年神经系统中的功能已经得到很好的证实,但前神经递生素在发育和损伤诱导的细胞死亡以及突触可塑性中的作用直到最近才被认识到。有趣的是,成熟的神经递生素和前神经递生素都利用双受体复合物来介导其作用。成熟的神经递生素核心受体由 Trk 受体酪氨酸激酶和 p75(NTR)组成,其中 Trk 转导生存和分化信号,而 p75(NTR)调节 Trk 激活的亲和力和选择性。另一方面,前神经递生素与 p75(NTR)和结构上不同的核心受体分选素结合,启动 p75(NTR)依赖性信号转导级联。尽管成熟的神经递生素与前神经递生素作用的特异性部分归因于形成不同的核心受体复合物,但最近的许多研究强调了如何调节不同的 p75(NTR)介导的细胞作用。在这里,我们回顾了关于配体特异性 p75(NTR)激活的新的跨膜机制的新证据,以及几种选择性激活 p75(NTR)依赖性凋亡和非凋亡反应的机制。

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