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The Hsc66-Hsc20 chaperone system in Escherichia coli: chaperone activity and interactions with the DnaK-DnaJ-grpE system.大肠杆菌中的Hsc66-Hsc20伴侣系统:伴侣活性及与DnaK-DnaJ-grpE系统的相互作用
J Bacteriol. 1998 Dec;180(24):6617-24. doi: 10.1128/JB.180.24.6617-6624.1998.
2
Hsc66 and Hsc20, a new heat shock cognate molecular chaperone system from Escherichia coli.Hsc66和Hsc20,一种来自大肠杆菌的新型热休克同源分子伴侣系统。
Protein Sci. 1997 May;6(5):1047-56. doi: 10.1002/pro.5560060511.
3
Regulation of ATPase and chaperone cycle of DnaK from Thermus thermophilus by the nucleotide exchange factor GrpE.嗜热栖热菌中核苷酸交换因子GrpE对DnaK的ATP酶及伴侣循环的调控
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4
Interaction of the iron-sulfur cluster assembly protein IscU with the Hsc66/Hsc20 molecular chaperone system of Escherichia coli.铁硫簇组装蛋白IscU与大肠杆菌Hsc66/Hsc20分子伴侣系统的相互作用。
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5
ClpB cooperates with DnaK, DnaJ, and GrpE in suppressing protein aggregation. A novel multi-chaperone system from Escherichia coli.ClpB与DnaK、DnaJ和GrpE协同作用以抑制蛋白质聚集。一种来自大肠杆菌的新型多分子伴侣系统。
J Biol Chem. 1999 Oct 1;274(40):28083-6. doi: 10.1074/jbc.274.40.28083.
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Complementation studies of the DnaK-DnaJ-GrpE chaperone machineries from Vibrio harveyi and Escherichia coli, both in vivo and in vitro.对哈维氏弧菌和大肠杆菌的DnaK-DnaJ-GrpE伴侣蛋白机器进行体内和体外互补研究。
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7
Real time kinetics of the DnaK/DnaJ/GrpE molecular chaperone machine action.DnaK/DnaJ/GrpE分子伴侣机器作用的实时动力学
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8
A cycle of binding and release of the DnaK, DnaJ and GrpE chaperones regulates activity of the Escherichia coli heat shock transcription factor sigma32.DnaK、DnaJ和GrpE分子伴侣的结合与释放循环调节大肠杆菌热休克转录因子sigma32的活性。
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Contributions of the LPPVK motif of the iron-sulfur template protein IscU to interactions with the Hsc66-Hsc20 chaperone system.铁硫模板蛋白IscU的LPPVK基序与Hsc66-Hsc20伴侣系统相互作用的贡献。
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10
The power stroke of the DnaK/DnaJ/GrpE molecular chaperone system.DnaK/DnaJ/GrpE分子伴侣系统的动力冲程。
J Mol Biol. 1997 Jun 27;269(5):757-68. doi: 10.1006/jmbi.1997.1072.

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The role of chaperones in iron-sulfur cluster biogenesis.伴侣蛋白在铁硫簇生物发生中的作用。
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Regulation of human Nfu activity in Fe-S cluster delivery-characterization of the interaction between Nfu and the HSPA9/Hsc20 chaperone complex.在 Fe-S 簇递送上调节人 Nfu 活性-鉴定 Nfu 与 HSPA9/Hsc20 伴侣复合物之间的相互作用。
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Partner proteins determine multiple functions of Hsp70.伴侣蛋白决定热休克蛋白70的多种功能。
Trends Cell Biol. 1995 May;5(5):207-12. doi: 10.1016/s0962-8924(00)89001-7.
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Assembly of iron-sulfur clusters. Identification of an iscSUA-hscBA-fdx gene cluster from Azotobacter vinelandii.铁硫簇的组装。从棕色固氮菌中鉴定出iscSUA-hscBA-fdx基因簇。
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Sequence analysis of a 34.7-kb DNA segment from the genome of Buchnera aphidicola (endosymbiont of aphids) containing groEL, dnaA, the atp operon, gidA, and rho.对来自蚜虫内共生菌蚜虫内共生菌基因组的一段34.7 kb DNA片段进行序列分析,该片段包含groEL、dnaA、atp操纵子、gidA和rho。
Curr Microbiol. 1998 Mar;36(3):158-63. doi: 10.1007/pl00006760.
4
The conserved carboxyl terminus and zinc finger-like domain of the co-chaperone Ydj1 assist Hsp70 in protein folding.共伴侣蛋白Ydj1保守的羧基末端和锌指样结构域协助热休克蛋白70进行蛋白质折叠。
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The Hsp70 and Hsp60 chaperone machines.热休克蛋白70(Hsp70)和热休克蛋白60(Hsp60)伴侣机制。
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7
In vitro evidence that hsp90 contains two independent chaperone sites.体外实验证据表明热休克蛋白90包含两个独立的伴侣蛋白位点。
FEBS Lett. 1997 Nov 24;418(1-2):139-43. doi: 10.1016/s0014-5793(97)01363-x.
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10
Crystallization and preliminary X-ray crystallographic properties of Hsc20, a J-motif co-chaperone protein from Escherichia coli.来自大肠杆菌的J基序共伴侣蛋白Hsc20的结晶及初步X射线晶体学性质
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大肠杆菌中的Hsc66-Hsc20伴侣系统:伴侣活性及与DnaK-DnaJ-grpE系统的相互作用

The Hsc66-Hsc20 chaperone system in Escherichia coli: chaperone activity and interactions with the DnaK-DnaJ-grpE system.

作者信息

Silberg J J, Hoff K G, Vickery L E

机构信息

Department of Physiology and Biophysics, University of California, Irvine, California 92697, USA.

出版信息

J Bacteriol. 1998 Dec;180(24):6617-24. doi: 10.1128/JB.180.24.6617-6624.1998.

DOI:10.1128/JB.180.24.6617-6624.1998
PMID:9852006
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC107765/
Abstract

Hsc66, a stress-70 protein, and Hsc20, a J-type accessory protein, comprise a newly described Hsp70-type chaperone system in addition to DnaK-DnaJ-GrpE in Escherichia coli. Because endogenous substrates for the Hsc66-Hsc20 system have not yet been identified, we investigated chaperone-like activities of Hsc66 and Hsc20 by their ability to suppress aggregation of denatured model substrate proteins, such as rhodanese, citrate synthase, and luciferase. Hsc66 suppressed aggregation of rhodanese and citrate synthase, and ATP caused effects consistent with complex destabilization typical of other Hsp70-type chaperones. Differences in the activities of Hsc66 and DnaK, however, suggest that these chaperones have dissimilar substrate specificity profiles. Hsc20, unlike DnaJ, did not exhibit intrinsic chaperone activity and appears to function solely as a regulatory cochaperone protein for Hsc66. Possible interactions between the Hsc66-Hsc20 and DnaK-DnaJ-GrpE chaperone systems were also investigated by measuring the effects of cochaperone proteins on Hsp70 ATPase activities. The nucleotide exchange factor GrpE did not stimulate the ATPase activity of Hsc66 and thus appears to function specifically with DnaK. Cross-stimulation by the cochaperones Hsc20 and DnaJ was observed, but the requirement for supraphysiological concentrations makes it unlikely that these interactions occur significantly in vivo. Together these results suggest that Hsc66-Hsc20 and DnaK-DnaJ-GrpE comprise separate molecular chaperone systems with distinct, nonoverlapping cellular functions.

摘要

Hsc66是一种应激70蛋白,Hsc20是一种J型辅助蛋白,它们在大肠杆菌中构成了一种新描述的Hsp70型伴侣系统,此外还有DnaK-DnaJ-GrpE。由于尚未确定Hsc66-Hsc20系统的内源性底物,我们通过Hsc66和Hsc20抑制变性模型底物蛋白(如硫氰酸酶、柠檬酸合酶和荧光素酶)聚集的能力,研究了它们的伴侣样活性。Hsc66抑制了硫氰酸酶和柠檬酸合酶的聚集,并且ATP产生的效应与其他Hsp70型伴侣典型的复合物不稳定一致。然而,Hsc66和DnaK活性的差异表明这些伴侣具有不同的底物特异性谱。与DnaJ不同,Hsc20没有表现出内在的伴侣活性,似乎仅作为Hsc66的调节性共伴侣蛋白发挥作用。我们还通过测量共伴侣蛋白对Hsp70 ATP酶活性的影响,研究了Hsc66-Hsc20和DnaK-DnaJ-GrpE伴侣系统之间可能的相互作用。核苷酸交换因子GrpE没有刺激Hsc66的ATP酶活性,因此似乎专门与DnaK起作用。观察到共伴侣Hsc20和DnaJ之间的交叉刺激,但由于需要超生理浓度,这些相互作用在体内不太可能显著发生。这些结果共同表明,Hsc66-Hsc20和DnaK-DnaJ-GrpE构成了具有不同且不重叠细胞功能的独立分子伴侣系统。