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Molecular mechanisms of HipA-mediated multidrug tolerance and its neutralization by HipB.


ABSTRACT: Bacterial multidrug tolerance is largely responsible for the inability of antibiotics to eradicate infections and is caused by a small population of dormant bacteria called persisters. HipA is a critical Escherichia coli persistence factor that is normally neutralized by HipB, a transcription repressor, which also regulates hipBA expression. Here, we report multiple structures of HipA and a HipA-HipB-DNA complex. HipA has a eukaryotic serine/threonine kinase-like fold and can phosphorylate the translation factor EF-Tu, suggesting a persistence mechanism via cell stasis. The HipA-HipB-DNA structure reveals the HipB-operator binding mechanism, approximately 70 degrees DNA bending, and unexpected HipA-DNA contacts. Dimeric HipB interacts with two HipA molecules to inhibit its kinase activity through sequestration and conformational inactivation. Combined, these studies suggest mechanisms for HipA-mediated persistence and its neutralization by HipB.

SUBMITTER: Schumacher MA 

PROVIDER: S-EPMC2764309 | biostudies-literature | 2009 Jan

REPOSITORIES: biostudies-literature

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Molecular mechanisms of HipA-mediated multidrug tolerance and its neutralization by HipB.

Schumacher Maria A MA   Piro Kevin M KM   Xu Weijun W   Hansen Sonja S   Lewis Kim K   Brennan Richard G RG  

Science (New York, N.Y.) 20090101 5912


Bacterial multidrug tolerance is largely responsible for the inability of antibiotics to eradicate infections and is caused by a small population of dormant bacteria called persisters. HipA is a critical Escherichia coli persistence factor that is normally neutralized by HipB, a transcription repressor, which also regulates hipBA expression. Here, we report multiple structures of HipA and a HipA-HipB-DNA complex. HipA has a eukaryotic serine/threonine kinase-like fold and can phosphorylate the t  ...[more]

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