4.6 Article

Evidence-Based Structural Model of the Staphylococcal Repressor Protein: Separation of Functions into Different Domains

期刊

PLOS ONE
卷 10, 期 9, 页码 -

出版社

PUBLIC LIBRARY SCIENCE
DOI: 10.1371/journal.pone.0139086

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资金

  1. Hungarian Scientific Research Fund OTKA [NK 84008, K109486]
  2. Baross Program of the New Hungary Development Plan [3DSTRUCT] [OMFB-00266/2010 REG-KM- 09-1-2009-0050]
  3. Hungarian Academy of Sciences [TTK IF-28/2012]
  4. Hungarian Academy of Sciences (MedinProt program)
  5. ICGEB Research Grant [CRP/HUN14-01]
  6. European Commission FP7 Biostruct-X project [283570]
  7. Hungarian Academy of Sciences
  8. [KTIA_NAP_13-2-2014-0017]

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Horizontal transfer of mobile genetic elements within Staphylococci is of high biomedical significance as such elements are frequently responsible for virulence and toxic effects. Staphylococcus-encoded repressor proteins regulate the replication of these mobile genetic elements that are located within the so-called pathogenicity islands. Here, we report structural and functional characterization of one such repressor protein, namely the Stl protein encoded by the pathogenicity island SaPIbov1. We create a 3D structural model and based on this prediction, we investigate the different functionalities of truncated and point mutant constructs. Results suggest that a helix-turn-helix motif governs the interaction of the Stl protein with its cognate DNA site: point mutations within this motif drastically decrease DNA-binding ability, whereas the interaction with the Stl-binding partner protein dUTPase is unperturbed by these point mutations. The 3D model also suggested the potential independent folding of a carboxy-terminal domain. This suggestion was fully verified by independent experiments revealing that the carboxy-terminal domain does not bind to DNA but is still capable of binding to and inhibiting dUTPase. A general model is proposed, which suggests that among the several structurally different repressor superfamilies Stl-like Staphylococcal repressor proteins belong to the helix-turn-helix transcription factor group and the HTH motif is suggested to reside within N-terminal segment.

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