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解旋酶 DnaK 伴侣蛋白与核苷酸/底物结合的构象。

The nucleotide-bound/substrate-bound conformation of the Mycoplasma genitalium DnaK chaperone.

机构信息

Instituto de Biología Molecular de Barcelona (IBMB-CSIC), Parc Científic de Barcelona, Barcelona, Spain.

Structural Biology Group, European Synchrotron Radiation Facility, CS 40220, Grenoble, France and ALBA Synchrotron, Carrer de la Llum 2-26, 08290 Cerdanyola del Vallès, Barcelona, Spain.

出版信息

Protein Sci. 2018 May;27(5):1000-1007. doi: 10.1002/pro.3401. Epub 2018 Apr 14.

Abstract

Hsp70 chaperones keep protein homeostasis facilitating the response of organisms to changes in external and internal conditions. Hsp70s have two domains-nucleotide binding domain (NBD) and substrate binding domain (SBD)-connected by a conserved hydrophobic linker. Functioning of Hsp70s depend on tightly regulated cycles of ATP hydrolysis allosterically coupled, often together with cochaperones, to the binding/release of peptide substrates. Here we describe the crystal structure of the Mycoplasma genitalium DnaK (MgDnaK) protein, an Hsp70 homolog, in the noncompact, nucleotide-bound/substrate-bound conformation. The MgDnaK structure resembles the one from the thermophilic eubacteria DnaK trapped in the same state. However, in MgDnaK the NBD and SBD domains remain close to each other despite the lack of direct interaction between them and with the linker contacting the two subdomains of SBD. These observations suggest that the structures might represent an intermediate of the protein where the conserved linker binds to the SBD to favor the noncompact state of the protein by stabilizing the SBDβ-SBDα subdomains interaction, promoting the capacity of the protein to sample different conformations, which is critical for proper functioning of the molecular chaperone allosteric mechanism. Comparison of the solved structures indicates that the NBD remains essentially invariant in presence or absence of nucleotide.

摘要

热休克蛋白 70(Hsp70)伴侣可以维持蛋白质的内环境稳定,促进生物体对外界和内部条件变化的适应。Hsp70 由两个结构域组成:核苷酸结合结构域(NBD)和底物结合结构域(SBD),它们由保守的疏水性连接子连接。Hsp70 的功能依赖于紧密调节的 ATP 水解循环,该循环通过变构与结合/释放肽底物偶联,通常与共伴侣一起作用。在这里,我们描述了支原体生殖道 DnaK(MgDnaK)蛋白的晶体结构,这是一种 Hsp70 同源物,处于非紧凑、核苷酸结合/底物结合构象。MgDnaK 结构类似于处于相同状态的嗜热真细菌 DnaK 的结构。然而,在 MgDnaK 中,尽管 NBD 和 SBD 结构域之间没有直接相互作用,而且连接子与 SBD 的两个亚结构域接触,但它们仍然彼此靠近。这些观察结果表明,这些结构可能代表蛋白质的中间状态,其中保守的连接子与 SBD 结合,通过稳定 SBDβ-SBDα 亚结构域的相互作用来促进蛋白质的非紧凑状态,从而提高蛋白质采样不同构象的能力,这对于分子伴侣变构机制的正常功能至关重要。与已解决结构的比较表明,NBD 在存在或不存在核苷酸的情况下基本保持不变。

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