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流感嗜血杆菌β-碳酸酐酶的变构位点变体

Allosteric site variants of Haemophilus influenzae beta-carbonic anhydrase.

作者信息

Rowlett Roger S, Tu Chingkuang, Lee Joseph, Herman Ariel G, Chapnick Douglas A, Shah Shalini H, Gareiss Peter C

机构信息

Department of Chemistry, Colgate University, 13 Oak Drive, Hamilton, New York 13346, USA.

出版信息

Biochemistry. 2009 Jul 7;48(26):6146-56. doi: 10.1021/bi900663h.

Abstract

Haemophilus influenzae beta-carbonic anhydrase (HICA) is hypothesized to be an allosteric protein that is regulated by the binding of bicarbonate ion to a non-catalytic (inhibitory) site that controls the ligation of Asp44 to the catalytically essential zinc ion. We report here the X-ray crystallographic structures of two variants (W39F and Y181F) involved in the binding of bicarbonate ion in the non-catalytic site and an active-site variant (D44N) that is incapable of forming a strong zinc ligand. The alteration of Trp39 to Phe increases the apparent K(i) for bicarbonate inhibition by 4.8-fold. While the structures of W39F and Y181F are very similar to the wild-type enzyme, the X-ray crystal structure of the D44N variant reveals that it has adopted an active-site conformation nearly identical to that of non-allosteric beta-carbonic anhydrases. We propose that the structure of the D44N variant is likely to be representative of the active conformation of the enzyme. These results lend additional support to the hypothesis that HICA is an allosteric enzyme that can adopt active and inactive conformations, the latter of which is stabilized by bicarbonate ion binding to a non-catalytic site.

摘要

流感嗜血杆菌β-碳酸酐酶(HICA)被推测为一种别构蛋白,它通过碳酸氢根离子与一个非催化(抑制性)位点的结合来调节,该位点控制着天冬氨酸44与催化必需的锌离子的连接。我们在此报告了两个参与碳酸氢根离子在非催化位点结合的变体(W39F和Y181F)以及一个无法形成强锌配体的活性位点变体(D44N)的X射线晶体结构。色氨酸39突变为苯丙氨酸使碳酸氢根抑制的表观K(i)增加了4.8倍。虽然W39F和Y181F的结构与野生型酶非常相似,但D44N变体的X射线晶体结构显示它采用了一种与非别构β-碳酸酐酶几乎相同的活性位点构象。我们提出D44N变体的结构可能代表了该酶的活性构象。这些结果为HICA是一种可以采用活性和非活性构象的别构酶这一假说提供了更多支持,其中非活性构象通过碳酸氢根离子与非催化位点的结合而稳定。

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