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Characterisation of the Plasmodium falciparum Hsp70–Hsp90 organising protein (PfHop)

机译:恶性疟原虫Hsp70–Hsp90组织蛋白(PfHop)的表征

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Malaria is caused by Plasmodium species, whose transmission to vertebrate hosts is facilitated by mosquito vectors. The transition from the cold blooded mosquito vector to the host represents physiological stress to the parasite, and additionally malaria blood stage infection is characterised by intense fever periods. In recent years, it has become clear that heat shock proteins play an essential role during the parasite's life cycle. Plasmodium falciparum expresses two prominent heat shock proteins: heat shock protein 70 (PfHsp70) and heat shock protein 90 (PfHsp90). Both of these proteins have been implicated in the development and pathogenesis of malaria. In eukaryotes, Hsp70 and Hsp90 proteins are functionally linked by an essential adaptor protein known as the Hsp70–Hsp90 organising protein (Hop). In this study, recombinant P. falciparum Hop (PfHop) was heterologously produced in E. coli and purified by nickel affinity chromatography. Using specific anti-PfHop antisera, the expression and localisation of PfHop in P. falciparum was investigated. PfHop was shown to co-localise with PfHsp70 and PfHsp90 in parasites at the trophozoite stage. Gel filtration and co-immunoprecipitation experiments suggested that PfHop was present in a complex together with PfHsp70 and PfHsp90. The association of PfHop with both PfHsp70 and PfHsp90 suggests that this protein may mediate the functional interaction between the two chaperones.
机译:疟疾是由疟原虫引起的,疟原虫通过蚊媒传播到脊椎动物宿主。从冷血蚊媒向宿主的过渡代表了对寄生虫的生理压力,此外,疟疾血液阶段感染的特征还在于高烧。近年来,已经清楚的是,热激蛋白在寄生虫的生命周期中起着至关重要的作用。恶性疟原虫表达两种突出的热激蛋白:热激蛋白70(PfHsp70)和热激蛋白90(PfHsp90)。这两种蛋白都与疟疾的发生和发病有关。在真核生物中,Hsp70和Hsp90蛋白通过称为Hsp70–Hsp90组织蛋白(Hop)的必需衔接子蛋白进行功能连接。在这项研究中,重组大肠杆菌恶性疟原虫(PfHop)是在大肠杆菌中异源产生的,并通过镍亲和层析纯化。使用特异性抗PfHop抗血清,研究了PfHop在恶性疟原虫中的表达和定位。在滋养体阶段,PfHop与PfHsp70和PfHsp90共同定位在寄生虫中。凝胶过滤和免疫共沉淀实验表明,PfHop与PfHsp70和PfHsp90一起存在于复合物中。 PfHop与PfHsp70和PfHsp90的缔合表明该蛋白可能介导两个分子伴侣之间的功能相互作用。

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