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动质体中热休克蛋白的后基因组学观点。

A postgenomic view of the heat shock proteins in kinetoplastids.

作者信息

Folgueira Cristina, Requena Jose M

机构信息

Centro de Biología Molecular Severo Ochoa, Universidad Autónoma de Madrid, Madrid, Spain.

出版信息

FEMS Microbiol Rev. 2007 Jul;31(4):359-77. doi: 10.1111/j.1574-6976.2007.00069.x. Epub 2007 Apr 25.

Abstract

The kinetoplastids Leishmania major, Trypanosoma brucei and Trypanosoma cruzi are causative agents of a diverse spectrum of human diseases: leishmaniasis, sleeping sickness and Chagas' disease, respectively. These protozoa possess digenetic life cycles that involve development in mammalian and insect hosts. It is generally accepted that temperature is a triggering factor of the developmental programme allowing the adaptation of the parasite to the mammalian conditions. The heat shock response is a general homeostatic mechanism that protects cells from the deleterious effects of environmental stresses, such as heat. This response is universal and includes the synthesis of the heat-shock proteins (HSPs). In this review, we summarize the salient features of the different HSP families and describe their main cellular functions. In parallel, we analyse the composition of these families in kinetoplastids according to literature data and our understanding of genome sequence data. The genome sequences of these parasites have been recently completed. The HSP families described here are: HSP110, HSP104, group I chaperonins, HSP90, HSP70, HSP40 and small HSPs. All these families are widely represented in these parasites. In particular, kinetoplastids possess an unprecedented number of members of the HSP70, HSP60 and HSP40 families, suggesting key roles for these HSPs in their biology.

摘要

动基体原虫硕大利什曼原虫、布氏锥虫和克氏锥虫分别是多种人类疾病的病原体:分别引起利什曼病、昏睡病和恰加斯病。这些原生动物具有双宿主生活周期,涉及在哺乳动物宿主和昆虫宿主中的发育。一般认为温度是发育程序的触发因素,使寄生虫能够适应哺乳动物环境。热休克反应是一种普遍的稳态机制,可保护细胞免受环境压力(如热)的有害影响。这种反应是普遍存在的,包括热休克蛋白(HSP)的合成。在本综述中,我们总结了不同HSP家族的显著特征,并描述了它们的主要细胞功能。同时,我们根据文献数据以及我们对基因组序列数据的理解,分析了动基体原虫中这些家族的组成。这些寄生虫的基因组序列最近已完成。这里描述的HSP家族包括:HSP110、HSP104、Ⅰ型伴侣蛋白、HSP90、HSP70、HSP40和小分子HSP。所有这些家族在这些寄生虫中都有广泛的代表。特别是,动基体原虫拥有数量空前的HSP70、HSP60和HSP40家族成员,表明这些HSP在其生物学中起关键作用。

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