Please use this identifier to cite or link to this item: http://hdl.handle.net/10397/118352
DC FieldValueLanguage
dc.contributorDepartment of Applied Biology and Chemical Technology-
dc.contributorResearch Centre for Chinese Medicine Innovation-
dc.contributorMainland Development Office-
dc.contributorDepartment of Food Science and Nutrition-
dc.contributorUniversity Research Facility in Life Sciences-
dc.creatorHuang, L-
dc.creatorWong, TF-
dc.creatorCheng, Q-
dc.creatorSo, PK-
dc.creatorLiu, M-
dc.creatorLi, X-
dc.creatorChen, S-
dc.creatorYao, ZP-
dc.date.accessioned2026-04-08T09:01:39Z-
dc.date.available2026-04-08T09:01:39Z-
dc.identifier.issn0002-7863-
dc.identifier.urihttp://hdl.handle.net/10397/118352-
dc.language.isoenen_US
dc.publisherAmerican Chemical Societyen_US
dc.titleInhibitor-dependent tolerance of New Delhi metallo-β-lactamase driven by single mutation-induced conformational changesen_US
dc.typeJournal/Magazine Articleen_US
dc.identifier.spage26389-
dc.identifier.epage26401-
dc.identifier.volume147-
dc.identifier.issue30-
dc.identifier.doi10.1021/jacs.5c05669-
dcterms.abstractThe emergence of metallo-β-lactamases as formidable adversaries in the antimicrobial resistance crisis stems from their unparalleled capacity to hydrolyze β-lactam antibiotics. This study deciphers the evolutionary strategy of New Delhi metallo-β-lactamase (NDM) variants through studies of conformational dynamics. We employ hydrogen/deuterium exchange mass spectrometry (HDX-MS) to map conformational landscapes of NDM in the ligand-free state and in the bound states with inhibitors l-captopril, d-captopril, ebselen, and aspergillomarasmine A (AMA), respectively. Crucially, our findings reveal similar allosteric fingerprints corresponding to different inhibition mechanisms; that is, inhibition induces pronounced dynamic perturbations in the α3–L8–β8 region─a previously under-characterized region. Strikingly, the clinically prevalent M154L mutation in this region reshapes conformational flexibility, amplifying inhibitor-specific conformational responses without altering the l/d-captopril binding dynamics. This study demonstrates how a single mutation can be critical for antibiotic resistance evolution where zinc is scarce in the presence of AMA and ebselen, as indicated by more protected HDX patterns of the α3–L8 region and several active-site loop (ASL) regions. Our results establish three key advances: (1) identification of α3–L8 as a cryptic allosteric region governing conformational adaptability, (2) demonstration of a single mutation M154L rewiring long-range dynamic communication, and (3) proposal of conformation-guided inhibitor design as a viable strategy against NDM. Overall, this work unveils a novel perspective─resistance mutations function not merely as chemical optimizers but as allosteric modulators that exploit inherent protein plasticity. These insights position the α3–L8 region as a compelling target for developing novel inhibitors, providing a blueprint for combating the next frontier of antimicrobial resistance.-
dcterms.accessRightsembargoed accessen_US
dcterms.bibliographicCitationJournal of the American Chemical Society, 30 July 2025, v. 147, no. 30, p. 26389-26401-
dcterms.isPartOfJournal of the American Chemical Society-
dcterms.issued2025-07-30-
dc.identifier.scopus2-s2.0-105012782611-
dc.identifier.pmid40690763-
dc.identifier.eissn1520-5126-
dc.description.validate202604 bcjz-
dc.description.oaNot applicableen_US
dc.identifier.SubFormIDG001400/2026-03en_US
dc.description.fundingSourceRGCen_US
dc.description.fundingSourceOthersen_US
dc.description.fundingTextWe thank other members in the Yao group for their helpful discussion. This work was supported by the National Key Research and Development Program of China (Grant No. 2024YFF0725800), the National Science Foundation of China (Grant No. 82304439), the China Postdoctoral Science Foundation (Grant No. 2023M743067), and the Hong Kong Research Grants Council (Grant Nos. 15304117, 15306421, R5013-19, C5026-24G, C5031-14E, C4014-23G, T11-104/22-R, SRFS2324-7S01, and CRS_CUHK405/23). We thank the University Research Facility in Life Sciences, the University Research Facility in Chemical and Environmental Analysis of The Hong Kong Polytechnic University, and the Core Facilities of Jinhua Institute of Zhejiang University for the technical and instrumental support. We also like to acknowledge Dr. Shan Feng’s team from Biomedical Research Core Facilities of Westlake University for instrumental support.en_US
dc.description.pubStatusPublisheden_US
dc.date.embargo2026-07-21en_US
dc.description.oaCategoryGreen (AAM)en_US
Appears in Collections:Journal/Magazine Article
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