多质子化HIV-1蛋白酶-配体复合物的计算滴定分析

Computational titration analysis of a multiprotic HIV-1 protease-ligand complex.

作者信息

Spyrakis Francesca, Fornabaio Micaela, Cozzini Pietro, Mozzarelli Andrea, Abraham Donald J, Kellogg Glen E

机构信息

Department of Biochemistry and Molecular Biology, University of Parma, 43100, Italy.

出版信息

J Am Chem Soc. 2004 Sep 29;126(38):11764-5. doi: 10.1021/ja0465754.

DOI:10.1021/ja0465754

PMID:15382890

Abstract

A new computational method for analyzing the protonation states of protein-ligand complexes with multiple ionizable groups is applied to the structurally characterized complex between the peptide Glu-Asp-Leu and HIV-1 protease. This complex has eight ionizable groups at the active site: four from the ligand and four Asp residues on the protein. Correlation, with an error of ca. 0.6 kcal mol-1, is made between the calculated titration curve and the experimental titration curve. The analysis suggests that between four and five of the eight ionizable groups are protonated at the pH of crystallization.

摘要

一种用于分析具有多个可电离基团的蛋白质-配体复合物质子化状态的新计算方法，被应用于结构已明确的肽Glu-Asp-Leu与HIV-1蛋白酶之间的复合物。该复合物在活性位点有八个可电离基团：四个来自配体，四个是蛋白质上的天冬氨酸残基。计算得到的滴定曲线与实验滴定曲线之间具有相关性，误差约为0.6千卡/摩尔。分析表明，在结晶pH值下，八个可电离基团中有四到五个处于质子化状态。

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多质子化HIV-1蛋白酶-配体复合物的计算滴定分析

Computational titration analysis of a multiprotic HIV-1 protease-ligand complex.

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