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詹氏甲烷球菌小热休克蛋白伴侣活性的机制

On the mechanism of chaperone activity of the small heat-shock protein of Methanococcus jannaschii.

作者信息

Kim Rosalind, Lai Luhua, Lee Hi-Hong, Cheong Gang-Won, Kim Kyeong Kyu, Wu Zheng, Yokota Hisao, Marqusee Susan, Kim Sung-Hou

机构信息

Physical Biosciences Division, Lawrence Berkeley National Laboratory, Berkeley, CA 94720, USA.

出版信息

Proc Natl Acad Sci U S A. 2003 Jul 8;100(14):8151-5. doi: 10.1073/pnas.1032940100. Epub 2003 Jun 19.

Abstract

The small heat-shock protein (sHSP) from Methanococcus jannaschii (Mj HSP16.5) forms a homomeric complex of 24 subunits and has an overall structure of a multiwindowed hollow sphere with an external diameter of approximately 120 A and an internal diameter of approximately 65 A with six square "windows" of approximately 17 A across and eight triangular windows of approximately 30 A across. This sHSP has been known to protect other proteins from thermal denaturation. Using purified single-chain monellin as a substrate and a series of methods such as protease digestion, antibody binding, and electron microscopy, we show that the substrates bind to Mj HSP16.5 at a high temperature (80 degrees C) on the outside surface of the sphere and are prevented from forming insoluble substrate aggregates in vitro. Circular dichroism studies suggest that a very small, if any, conformational change occurs in sHSP even at 80 degrees C, but substantial conformational changes of the substrate are required for complex formation at 80 degrees C. Furthermore, deletion mutation studies of Mj HSP16.5 suggest that the N-terminal region of the protein has no structural role but may play an important kinetic role in the assembly of the sphere by "preassembly condensation" of multiple monomers before final assembly of the sphere.

摘要

詹氏甲烷球菌的小分子热休克蛋白(Mj HSP16.5)形成由24个亚基组成的同聚复合物,其整体结构为多窗口空心球体,外径约120埃,内径约65埃,有六个边长约17埃的方形“窗口”和八个边长约30埃的三角形窗口。已知这种小分子热休克蛋白能保护其他蛋白质免受热变性影响。我们以纯化的单链莫内林为底物,采用蛋白酶消化、抗体结合及电子显微镜等一系列方法,证明底物在高温(80℃)下结合于球体外侧表面的Mj HSP16.5,且在体外可防止形成不溶性底物聚集体。圆二色性研究表明,即便在80℃时,小分子热休克蛋白发生的构象变化(如果有的话)也非常小,但在80℃形成复合物时底物需要发生显著的构象变化。此外,对Mj HSP16.5的缺失突变研究表明,该蛋白的N端区域不具有结构作用,但可能在球体组装过程中通过多个单体在球体最终组装前的“预组装凝聚”发挥重要的动力学作用。

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