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首页> 外文期刊>Journal of Molecular Biology >Functional similarities and differences of an archaeal Hsp70(DnaK) stress protein compared with its homologue from the bacterium Escherichia coli.
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Functional similarities and differences of an archaeal Hsp70(DnaK) stress protein compared with its homologue from the bacterium Escherichia coli.

机译:与古细菌Hsp70(DnaK)应激蛋白的同源物相比,其功能相似性和差异。

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摘要

Archaea are prokaryotes but some of their chaperoning systems resemble those of eukaryotes. Also, not all archaea possess the stress protein Hsp70(DnaK), in contrast with bacteria and eukaryotes, which possess it without any known exception. Further, the primary structure of the archaeal DnaK resembles more the bacterial than the eukaryotic homologues. The work reported here addresses two questions: Is the archaeal Hsp70 protein a chaperone, like its homologues in the other two phylogenetic domains? And, if so, is the chaperoning mechanism of bacterial or eukaryotic type? The data have shown that the DnaK protein of the archaeon Methanosarcina mazei functions efficiently as a chaperone in luciferase renaturation in vitro, and that it requires DnaJ, and the other bacterial-type chaperone, GrpE, to perform its function. The M. mazei DnaK chaperone activity was enhanced by interaction with the bacterial co-chaperone DnaJ, but not by the eukaryotic homologue HDJ-2. Both the bacterial GrpE and DnaJ stimulated the ATPase activity of the M. mazei DnaK. The M. mazei DnaK-dependent chaperoning pathway in vitro is similar to that of the bacterium Escherichia coli used for comparison. However, in vivo analyses indicate that there are also significant differences. The M. mazei dnaJ and grpE genes rescued E.coli mutants lacking these genes, but E.coli dnaK mutants were not complemented by the M. mazei dnaK gene. Thus, while the data from in vitro tests demonstrate functional similarities between the M. mazei and E.coli DnaK proteins, in vivo results indicate that, intracellularly, the chaperones from the two species differ.
机译:古细菌是原核生物,但它们的一些陪伴系统类似于真核生物。而且,与细菌和真核生物相反,并非所有古细菌都具有应激蛋白Hsp70(DnaK),而细菌和真核生物没有任何已知例外。此外,古细菌DnaK的一级结构比真核同源物更像细菌。此处报道的工作解决了两个问题:古细菌Hsp70蛋白是伴侣蛋白吗,就像其在其他两个系统发育域中的同系物一样?而且,如果是的话,细菌或真核生物的伴侣机制是吗?数据表明,古细菌甲烷八叠球菌的DnaK蛋白在体外萤光素酶复性中有效地作为伴侣蛋白起作用,它需要DnaJ和其他细菌型伴侣蛋白GrpE来发挥其功能。通过与细菌伴侣伴侣DnaJ的相互作用增强了马氏甲烷八叠球菌的DnaK伴侣活性,但通过真核同源物HDJ-2却没有。细菌GrpE和DnaJ都刺激了马氏甲烷八叠球菌DnaK的ATPase活性。体外M. mazei DnaK伴侣伴侣途径与用于比较的大肠杆菌相似。但是,体内分析表明也存在显着差异。 M. mazei dnaJ和grpE基因拯救了缺少这些基因的E.coli突变体,但是E.coli dnaK突变体没有M. mazei dnaK基因的补充。因此,尽管来自体外试验的数据证明了马氏甲烷八叠球菌和大肠杆菌DnaK蛋白之间的功能相似性,但体内结果表明,在细胞内,这两个物种的分子伴侣不同。

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