AI Article Synopsis

  • New Delhi metallo-β-lactamase (NDM) is a significant global threat due to its resistance to critical antibiotics, and new variants like NDM-15 show enhanced resilience to low zinc levels.
  • A novel fluorescent probe has been created to track the metalation state of NDM, significantly increasing fluorescence intensity and allowing for detailed studies of enzyme behavior.
  • This tool aids in understanding how metal ion levels affect NDM's resistance and could help develop new therapies to combat antibiotic resistance.

Article Abstract

New Delhi metallo-β-lactamase (NDM) grants resistance to a broad spectrum of β-lactam antibiotics, including last-resort carbapenems, and is emerging as a global antibiotic resistance threat. Limited zinc availability adversely impacts the ability of NDM-1 to provide resistance, but a number of clinical variants have emerged that are more resistant to zinc scarcity (e.g., NDM-15). To provide a novel tool to better study metal ion sequestration in host-pathogen interactions, we describe the development of a fluorescent probe that reports on the dynamic metalation state of NDM within . The thiol-containing probe selectively coordinates the dizinc metal cluster of NDM and results in a 17-fold increase in fluorescence intensity. Reversible binding enables competition and time-dependent studies that reveal fluorescence changes used to detect enzyme localization, substrate and inhibitor engagement, and changes to metalation state through the imaging of live using confocal microscopy. NDM-1 is shown to be susceptible to demetalation by intracellular and extracellular metal chelators in a live-cell model of zinc dyshomeostasis, whereas the NDM-15 metalation state is shown to be more resistant to zinc flux. The development of this reversible turn-on fluorescent probe for the metalation state of NDM provides a new tool for monitoring the impact of metal ion sequestration by host defense mechanisms and for detecting inhibitor-target engagement during the development of therapeutics to counter this resistance determinant.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8230704PMC
http://dx.doi.org/10.1021/jacs.1c00290DOI Listing

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