AI Article Synopsis

  • NsaS is an intramembrane histidine kinase in Staphylococcus aureus, playing a crucial role in the bacteria's defense against antimicrobials and human immune responses.* -
  • The study utilizes advanced techniques like NMR spectroscopy and molecular modeling to uncover three main structural features of NsaS: an N-terminal helix that helps anchor it in the membrane, a dynamic transmembrane domain, and a flexible linker to its catalytic domains.* -
  • The intracellular linker is particularly interesting, showing variability in its structure that might change during antibiotic signaling, indicating how NsaS adapts during interactions with antibiotics.*

Article Abstract

NsaS is one of four intramembrane histidine kinases (HKs) in Staphylococcus aureus that mediate the pathogen's response to membrane active antimicrobials and human innate immunity. We describe the first integrative structural study of NsaS using a combination of solution state NMR spectroscopy, chemical-cross-linking, molecular modeling and dynamics. Three key structural features emerge: First, NsaS has a short N-terminal amphiphilic helix that anchors its transmembrane (TM) bundle into the inner leaflet of the membrane such that it might sense neighboring proteins or membrane deformations. Second, the transmembrane domain of NsaS is a 4-helix bundle with significant dynamics and structural deformations at the membrane interface. Third, the intracellular linker connecting the TM domain to the cytoplasmic catalytic domains of NsaS is a marginally stable helical dimer, with one state likely to be a coiled-coil. Data from chemical shifts, heteronuclear NOE, H/D exchange measurements and molecular modeling suggest that this linker might adopt different conformations during antibiotic induced signaling.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6499544PMC
http://dx.doi.org/10.1021/jacs.7b09670DOI Listing

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