5NBK

NDM-1 metallo-beta-lactamase: a parsimonious interpretation of the diffraction data

5NBK の概要

• エントリーDOI: 10.2210/pdb5nbk/pdb
• 分子名称: Metallo-beta-lactamase type 2, ZINC ION, TETRAETHYLENE GLYCOL, ... (6 entities in total)
• 機能のキーワード: hydrolase, ndm-1, metallo-beta-lactamase
• 由来する生物種: Klebsiella pneumoniae
• タンパク質・核酸の鎖数: 2
• 化学式量合計: 54865.89

構造登録者

Raczynska, J.E.,Shabalin, I.G.,Jaskolski, M.,Minor, W.,Wlodawer, A. (登録日: 2017-03-02, 公開日: 2018-10-03, 最終更新日: 2024-05-08)

主引用文献

Raczynska, J.E.,Shabalin, I.G.,Minor, W.,Wlodawer, A.,Jaskolski, M.
A close look onto structural models and primary ligands of metallo-beta-lactamases.
Drug Resist. Updat., 40:1-12, 2018

PubMed Abstract: β-Lactamases are hydrolytic enzymes capable of opening the β-lactam ring of antibiotics such as penicillin, thus endowing the bacteria that produce them with antibiotic resistance. Of particular medical concern are metallo-β-lactamases (MBLs), with an active site built around coordinated Zn cations. MBLs are pan-reactive enzymes that can break down almost all classes of β-lactams, including such last-resort antibiotics as carbapenems. They are not only broad-spectrum-reactive but are often plasmid-borne (e.g., the New Delhi enzyme, NDM), and can spread horizontally even among unrelated bacteria. Acquired MBLs are encoded by mobile genetic elements, which often include other resistance genes, making the microbiological situation particularly alarming. There is an urgent need to develop MBL inhibitors in order to rescue our antibiotic armory. A number of such efforts have been undertaken, most notably using the 3D structures of various MBLs as drug-design targets. Structure-guided drug discovery depends on the quality of the structures that are collected in the Protein Data Bank (PDB) and on the consistency of the information in dedicated β-lactamase databases. We conducted a careful review of the crystal structures of class B β-lactamases, concluding that the quality of these structures varies widely, especially in the regions where small molecules interact with the macromolecules. In a number of examples the interpretation of the bound ligands (e.g., inhibitors, substrate/product analogs) is doubtful or even incorrect, and it appears that in some cases the modeling of ligands was not supported by electron density. For ten MBL structures, alternative interpretations of the original diffraction data could be proposed and the new models have been deposited in the PDB. In four cases, these models, prepared jointly with the authors of the original depositions, superseded the previous deposits. This review emphasizes the importance of critical assessment of structural models describing key drug design targets at the level of the raw experimental data. Since the structures reviewed here are the basis for ongoing design of new MBL inhibitors, it is important to identify and correct the problems with ambiguous crystallographic interpretations, thus enhancing reproducibility in this highly medically relevant area.

PubMed: 30466711
DOI: 10.1016/j.drup.2018.08.001

実験手法

X-RAY DIFFRACTION (2.6 Å)