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Colloquium Paper: The catalytic sites of 20S proteasomes and their role in subunit maturation: A mutational and crystallographic study

机译:专题讨论会:20S蛋白酶体的催化位点及其在亚基中的作用 成熟:突变和晶体学研究

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摘要

We present a biochemical and crystallographic characterization of active site mutants of the yeast 20S proteasome with the aim to characterize substrate cleavage specificity, subunit intermediate processing, and maturation. β1(Pre3), β2(Pup1), and β5(Pre2) are responsible for the postacidic, tryptic, and chymotryptic activity, respectively. The maturation of active subunits is independent of the presence of other active subunits and occurs by intrasubunit autolysis. The propeptides of β6(Pre7) and β7(Pre4) are intermediately processed to their final forms by β2(Pup1) in the wild-type enzyme and by β5(Pre2) and β1(Pre3) in the β2(Pup1) inactive mutants. A role of the propeptide of β1(Pre3) is to prevent acetylation and thereby inactivation. A gallery of proteasome mutants that contain active site residues in the context of the inactive subunits β3(Pup3), β6(Pre7), and β7(Pre4) show that the presence of Gly-1, Thr1, Asp17, Lys33, Ser129, Asp166, and Ser169 is not sufficient to generate activity.
机译:我们提出了酵母20S蛋白酶体活性位点突变体的生化和晶体学表征,目的是表征底物裂解特异性,亚基中间加工和成熟。 β1(Pre3),β2(Pup1)和β5(Pre2)分别负责酸性后,胰蛋白酶和糜蛋白酶的活性。活性亚基的成熟与其他活性亚基的存在无关,并且通过亚基内自溶而发生。 β6(Pre7)和β7(Pre4)的前肽在野生型酶中被β2(Pup1)以及在无活性的β2(Pup1)突变体中被β5(Pre2)和β1(Pre3)中间加工成最终形式。 β1(Pre3)的前肽的作用是防止乙酰化从而失活。包含在非活性亚基β3(Pup3),β6(Pre7)和β7(Pre4)中含有活性位点残基的蛋白酶体突变体的画廊显示,存在Gly-1,Thr1,Asp17,Lys33,Ser129,Asp166 ,而Ser169不足以产生活动。

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