A ‘through-DNA’ mechanism for co-regulation of metal uptake and efflux
Transition metals like Zn are essential for all organisms including bacteria, but fluctuations of their concentrations in the cell can be lethal. Organisms have thus evolved complex mechanisms for cellular metal homeostasis. One mechanistic paradigm involves pairs of transcription regulators sensing...
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Veröffentlicht in: | Nature communications 2024-12, Vol.15 (1), p.10555-11 |
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Zusammenfassung: | Transition metals like Zn are essential for all organisms including bacteria, but fluctuations of their concentrations in the cell can be lethal. Organisms have thus evolved complex mechanisms for cellular metal homeostasis. One mechanistic paradigm involves pairs of transcription regulators sensing intracellular metal concentrations to regulate metal uptake and efflux. Here we report that Zur and ZntR, a prototypical pair of regulators for Zn uptake and efflux in
E. coli
, respectively, can coordinate their regulation through DNA, besides sensing cellular Zn
2+
concentrations. Using a combination of live-cell single-molecule tracking and in vitro single-molecule FRET measurements, we show that unmetallated ZntR can enhance the unbinding kinetics of Zur from DNA by directly acting on Zur-DNA complexes, possibly through forming heteromeric ternary and quaternary complexes that involve both protein-DNA and protein-protein interactions. This ‘through-DNA’ mechanism may functionally facilitate the switching in Zn-uptake regulation when bacteria encounter changing Zn environments, such as facilitating derepression of Zn-uptake genes upon Zn depletion; it could also be relevant for regulating the uptake-vs.-efflux of various metals across different bacterial species and yeast.
Proteins Zur and ZntR sense intracellular zinc concentrations and regulate zinc transport, respectively, in
E. coli
. Here the authors show that the proteins coordinate their regulation through DNA, by forming heteromeric complexes that involve protein-DNA and protein-protein interactions. |
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ISSN: | 2041-1723 2041-1723 |
DOI: | 10.1038/s41467-024-55017-z |