Identification and Characterization of Noncovalent Interactions That Drive Binding and Specificity in DD-Peptidases and β-Lactamases

被引:13
作者
Hargis, Jacqueline C. [1 ]
Vankayala, Sai Lakshmana [1 ]
White, Justin K. [1 ]
Woodcock, H. Lee [1 ]
机构
[1] Univ S Florida, Dept Chem, Tampa, FL 33620 USA
关键词
GENERAL FORCE-FIELD; CROSS-LINKING; PENICILLIN; PEPTIDOGLYCAN; CHARMM; MECHANISM; PROBIS; QM/MM; SITE; RATIONALIZATION;
D O I
10.1021/ct400968v
中图分类号
O64 [物理化学(理论化学)、化学物理学];
学科分类号
070304 ; 081704 ;
摘要
Bacterial resistance to standard (i.e., beta-lactam-based) antibiotics has become a global pandemic. Simultaneously, research into the underlying causes of resistance has slowed substantially, although its importance is universally recognized. Key to unraveling critical details is characterization of the noncovalent interactions that govern binding and specificity (DD-peptidases, antibiotic targets, versus beta-lactamases, the evolutionarily derived enzymes that play a major role in resistance) and ultimately resistance as a whole. Herein, we describe a detailed investigation that elicits new chemical insights into these underlying intermolecular interactions. Benzylpenicillin and a novel beta-lactam peptidomimetic complexed to the Stremptomyces R61 peptidase are examined Using an arsenal of computational techniques: MD simulations, QM/MM calculations, charge perturbation analysis, QM/MM orbital analysis, bioinformatics, flexible receptor/flexible ligand docking, and computational ADME predictions. Several key molecular level interactions are identified that not only shed light onto fundamental resistance mechanisms, but also offer explanations for observed specificity. Specifically, an extended pi-pi network is elucidated that suggests antibacterial resistance has evolved, in part, due to stabilizing aromatic interactions. Additionally, interactions between the protein and peptidomimetic substrate are identified and characterized. Of particular interest is a water-mediated salt bridge between Asp217 and the positively charged N-terminus of the peptidomimetic, revealing an interaction that may significantly contribute to beta-lactam specificity. Finally, interaction information is used to suggest modifications to current beta-lactam compounds that should both improve binding and specificity in DD-peptidases and their physiochemical properties.
引用
收藏
页码:855 / 864
页数:10
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