26S和20S蛋白酶体的结构特征。

Enzyme & protein Pub Date : 1993-01-01 DOI:10.1159/000468684
A Lupas, A J Koster, W Baumeister
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引用次数: 94

摘要

26S蛋白酶体是蛋白质降解泛素依赖途径的中心蛋白酶,从黏菌到人类都具有高度保守的结构。细长分子由一个桶形20S核心配合物和两个极性19S配合物组成,分子量约为2000 kD。20S配合物具有C2对称性,由四个七元环组成,其中外环相对于内环旋转26度,而内环在寄存器中。19世纪盖层复合体是不对称的,因此在构造层面上的理解要少得多。通过比较26S和20S颗粒的活性和调控,可以推断20S颗粒含有蛋白酶活性,而19S复合物应该含有异肽酶、氧化还原酶、atp酶和蛋白展开活性。在这篇文章中,我们描述了各种蛋白酶体复合物的结构,通过电子显微镜确定,并讨论其亚基序列的结构含义。
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Structural features of 26S and 20S proteasomes.

The 26S proteasome is the central protease of the ubiquitin-dependent pathway of protein degradation and has a highly conserved structure from slime molds to humans. The elongated molecule which has a molecular mass of approximately 2,000 kD is formed by a barrel-shaped 20S core complex and two polar 19S complexes. The 20S complex has C2 symmetry and is built by four seven-membered rings of which the outer rings are rotated by 26 degrees relative to the inner rings while the inner rings are in register. The 19S cap complex is asymmetric and therefore considerably less well understood on a structural level. From a comparison of the activity and regulation of the 26S and 20S particles, it can be deduced that the 20S particle contains the protease activity while the 19S complex is supposed to contain isopeptidase, oxidoreductase, ATPase and protein-unfolding activities. In this article we describe the structure of various proteasome complexes as determined by electron microscopy and discuss structural implications of their subunit sequences.

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