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生死抉择:通过信号分子的蛋白水解作用对细胞凋亡进行调控

Life and death decisions: regulation of apoptosis by proteolysis of signaling molecules.

作者信息

Utz P J, Anderson P

机构信息

Stanford University School of Medicine, Department of Medicine, Division of Immunology and Rheumatology, Stanford, CA 94305, USA.

出版信息

Cell Death Differ. 2000 Jul;7(7):589-602. doi: 10.1038/sj.cdd.4400696.

Abstract

Caspases are the major executioners of cell death, serving as molecular guillotines to behead many proteins required for maintenance of cellular homeostasis. Identification of caspase substrates has taken on increasing importance as we attempt to better understand the molecular mechanisms involved in regulating the struggle between life and death. Many caspase substrates have been described and include RNA binding proteins such as La and U1-70 kD, structural proteins such as keratin and nuclear lamins, and transcription factors or their regulatory proteins that include IkappaB, SP1, and SREBP. Kinases and other signaling proteins are perfectly suited to regulate life and death decisions in response to cellular stressors and have only recently been identified as important caspase substrates. Here we review the current status of signaling pathways that are activated, inactivated or dysregulated by proteases such as caspases and calpain to control entry into apoptosis. The emerging concept that some caspase pathways may be inhibited by cellular and viral apoptosis inhibitory proteins while other caspase pathways are preserved suggests that a subset of these kinases may exist as cleaved 'isoforms' in cells that are not destined to perish. By acting as executioners and as important 'molecular sensors' of the degree of cellular injury, the signaling proteins described in this review are strong candidates to mediate downstream events, both in condemned and in viable cells.

摘要

半胱天冬酶是细胞死亡的主要执行者,充当分子断头台,切割许多维持细胞内稳态所需的蛋白质。随着我们试图更好地理解调节生死斗争所涉及的分子机制,鉴定半胱天冬酶底物变得越来越重要。已经描述了许多半胱天冬酶底物,包括RNA结合蛋白如La和U1 - 70 kD、结构蛋白如角蛋白和核纤层蛋白,以及转录因子或其调节蛋白,包括IkappaB、SP1和SREBP。激酶和其他信号蛋白非常适合响应细胞应激源调节生死决定,并且直到最近才被确定为重要的半胱天冬酶底物。在这里,我们综述了由半胱天冬酶和钙蛋白酶等蛋白酶激活、失活或失调以控制细胞凋亡进入的信号通路的现状。新出现的概念是,一些半胱天冬酶途径可能被细胞和病毒凋亡抑制蛋白抑制,而其他半胱天冬酶途径则得以保留,这表明这些激酶的一个子集可能以裂解的“异构体”形式存在于不会死亡的细胞中。作为细胞损伤程度的执行者和重要的“分子传感器”,本文所述的信号蛋白是介导注定死亡和存活细胞下游事件的有力候选者。

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