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Human, vector and parasite Hsp90 proteins: A comparative bioinformatics analysis

机译:人,载体和寄生虫Hsp90蛋白:比较性生物信息学分析

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The treatment of protozoan parasitic diseases is challenging, and thus identification and analysis of new drug targets is important. Parasites survive within host organisms, and some need intermediate hosts to complete their life cycle. Changing host environment puts stress on parasites, and often adaptation is accompanied by the expression of large amounts of heat shock proteins (Hsps). Among Hsps, Hsp90 proteins play an important role in stress environments. Yet, there has been little computational research on Hsp90 proteins to analyze them comparatively as potential parasitic drug targets. Here, an attempt was made to gain detailed insights into the differences between host, vector and parasitic Hsp90 proteins by large-scale bioinformatics analysis. A total of 104 Hsp90 sequences were divided into three groups based on their cellular localizations; namely cytosolic, mitochondrial and endoplasmic reticulum (ER). Further, the parasitic proteins were divided according to the type of parasite (protozoa, helminth and ectoparasite). Primary sequence analysis, phylogenetic tree calculations, motif analysis and physicochemical properties of Hsp90 proteins suggested that despite the overall structural conservation of these proteins, parasitic Hsp90 proteins have unique features which differentiate them from human ones, thus encouraging the idea that protozoan Hsp90 proteins should be further analyzed as potential drug targets.
机译:原生动物寄生虫病的治疗具有挑战性,因此新药靶标的鉴定和分析很重要。寄生虫可以在宿主生物体内生存,有些需要中间宿主才能完成其生命周期。不断变化的宿主环境给寄生虫带来了压力,并且适应过程通常伴随着大量热激蛋白(Hsps)的表达。在Hsps中,Hsp90蛋白在压力环境中起重要作用。然而,关于Hsp90蛋白作为潜在的寄生药物靶标进行比较分析的研究很少。在此,我们尝试通过大规模生物信息学分析来深入了解宿主,载体和寄生Hsp90蛋白之间的差异。根据它们的细胞定位,总共104个Hsp90序列被分成三组。即胞质,线粒体和内质网(ER)。此外,根据寄生虫的类型(原生动物,蠕虫和体外寄生虫)将寄生蛋白划分。 Hsp90蛋白质的初步序列分析,系统进化树计算,基序分析和理化性质表明,尽管Hsp90蛋白质具有整体结构保守性,但寄生Hsp90蛋白质仍具有独特的特征,可将它们与人的蛋白质区分开,因此鼓励人们认为应将原生动物Hsp90蛋白质进一步分析为潜在的药物靶标。

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