Crystal structures of SarA, a pleiotropic regulator of virulence genes in S. aureus
Maria A. Schumacher,
Barry K. Hurlburt and
Richard G. Brennan ()
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Maria A. Schumacher: Department of Biochemistry and Molecular Biology
Barry K. Hurlburt: University of Arkansas for Medical Sciences
Richard G. Brennan: Department of Biochemistry and Molecular Biology
Nature, 2001, vol. 409, issue 6817, 215-219
Abstract:
Abstract Staphylococcus aureus is a major human pathogen, the potency of which can be attributed to the regulated expression of an impressive array of virulence determinants. A key pleiotropic transcriptional regulator of these virulence factors is SarA, which is encoded by the sar (staphylococcal accessory regulator) locus1,2,3. SarA was characterized initially as an activator of a second virulence regulatory locus, agr, through its interaction with a series of heptad repeats (AGTTAAG) within the agr promoter4. Subsequent DNA-binding studies have revealed that SarA binds readily to multiple AT-rich sequences of variable lengths4,5,6,7,8,9,10,11. Here we describe the crystal structure of SarA and a SarA–DNA complex at resolutions of 2.50 Å and 2.95 Å, respectively. SarA has a fold consisting of a four-helix core region and ‘inducible regions’ comprising a β-hairpin and a carboxy-terminal loop. On binding DNA, the inducible regions undergo marked conformational changes, becoming part of extended and distorted α-helices, which encase the DNA. SarA recognizes an AT-rich site in which the DNA is highly overwound and adopts a D-DNA-like conformation by indirect readout. These structures thus provide insight into SarA-mediated transcription regulation.
Date: 2001
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DOI: 10.1038/35051623
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