Structural plasticity in Mycobacterium tuberculosis uracil-DNA glycosylase (MtUng) and its functional implications

被引:15
作者
Arif, S. M. [1 ]
Geethanandan, K. [1 ]
Mishra, P. [1 ]
Surolia, A. [1 ]
Varshney, U. [2 ]
Vijayan, M. [1 ]
机构
[1] Indian Inst Sci, Mol Biophys Unit, Bangalore 560012, Karnataka, India
[2] Indian Inst Sci, Dept Microbiol & Cell Biol, Bangalore 560012, Karnataka, India
来源
ACTA CRYSTALLOGRAPHICA SECTION D-STRUCTURAL BIOLOGY | 2015年 / 71卷
关键词
DNA repair; excision repair; ligand binding; molecular plasticity; conformational selection; BASE-EXCISION-REPAIR; COD GADUS-MORHUA; X-RAY-ANALYSIS; ESCHERICHIA-COLI; N-GLYCOSYLASE; CRYSTAL-STRUCTURE; INHIBITOR PROTEIN; MUTATIONAL ANALYSIS; COMPLEX; UNG;
D O I
10.1107/S1399004715009311
中图分类号
Q5 [生物化学];
学科分类号
071010 ; 081704 ;
摘要
17 independent crystal structures of family I uracil-DNA glycosylase from Mycobacterium tuberculosis (MtUng) and its complexes with uracil and its derivatives, distributed among five distinct crystal forms, have been determined. Thermodynamic parameters of binding in the complexes have been measured using isothermal titration calorimetry. The two-domain protein exhibits open and closed conformations, suggesting that the closure of the domain on DNA binding involves conformational selection. Segmental mobility in the enzyme molecule is confined to a 32-residue stretch which plays a major role in DNA binding. Uracil and its derivatives can bind to the protein in two possible orientations. Only one of them is possible when there is a bulky substituent at the 50 position. The crystal structures of the complexes provide a reasonable rationale for the observed thermodynamic parameters. In addition to providing fresh insights into the structure, plasticity and interactions of the protein molecule, the results of the present investigation provide a platform for structure-based inhibitor design.
引用
收藏
页码:1514 / 1527
页数:14
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