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The role of the DIF motif of the DnaJ (Hsp40) co-chaperone in the regulation of the DnaK (Hsp70) chaperone cycle

机译:DnaJ(Hsp40)伴侣伴侣的DIF主题在DnaK(Hsp70)伴侣周期调节中的作用

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摘要

To perform effectively as a molecular chaperone, DnaK (Hsp70) necessitates the assistance of its DnaJ (Hsp40) co-chaperone partner, which efficiently stimulates its intrinsically weak ATPase activity and facilitates its interaction with polypeptide substrates. In this study, we address the function of the conserved glycine- and phenylalanine-rich (G/F-rich) region of the Escherichia coli DnaJ in the DnaK chaperone cycle. We show that the G/F-rich region is critical for DnaJ co-chaperone functions in vivo and that despite a significant degree of sequence conservation among the G/F-rich regions of Hsp40 homologs from bacteria, yeast, or humans, functional complementation in the context of the E. coli DnaJ is limited. Furthermore, we found that the deletion of the whole G/F-rich region is mirrored by mutations in the conserved Asp-Ile/Val-Phe (DIF) motif contained in this region. Further genetic and biochemical analyses revealed that this amino acid triplet plays a critical role in regulation of the DnaK chaperone cycle, possibly by modulating a crucial step subsequent to DnaK-mediated ATP hydrolysis.
机译:为了有效地发挥分子伴侣的作用,DnaK(Hsp70)需要其DnaJ(Hsp40)伴侣伴侣的协助,该伴侣可以有效地刺激其固有的弱ATPase活性并促进其与多肽底物的相互作用。在这项研究中,我们解决了在DnaK分子伴侣循环中,大肠杆菌DnaJ的保守的富含甘氨酸和苯丙氨酸(富含G / F)的功能。我们显示,富含G / F的区域对于体内DnaJ伴侣分子的功能至关重要,尽管Hsp40同源物来自细菌,酵母或人类的Hsp40同源物的富含G / F的区域之间存在显着程度的序列保守性,但功能互补在大肠杆菌中,DnaJ是有限的。此外,我们发现整个富含G / F的区域的缺失被该区域所包含的保守Asp-Ile / Val-Phe(DIF)基序中的突变所反映。进一步的遗传和生化分析表明,该氨基酸三联体在调节DnaK分子伴侣循环中起着关键作用,可能是通过调节DnaK介导的ATP水解后的关键步骤来实现的。

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