Insight into the conformational stability of membrane-embedded BamA using a combined solution and solid-state NMR approach

被引:0
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作者
Tessa Sinnige
Klaartje Houben
Iva Pritisanac
Marie Renault
Rolf Boelens
Marc Baldus
机构
[1] Utrecht University,NMR Spectroscopy, Department of Chemistry, Faculty of Science, Bijvoet Center for Biomolecular Research
[2] Physical and Theoretical Chemistry Laboratory,undefined
[3] Institute of Pharmacology and Structural Biology,undefined
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关键词
NMR spectroscopy; Membrane proteins; Proteoliposomes; β-Barrel assembly; Protein dynamics;
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摘要
The β-barrel assembly machinery (BAM) is involved in folding and insertion of outer membrane proteins in Gram-negative bacteria, a process that is still poorly understood. With its 790 residues, BamA presents a challenge to current NMR methods. We utilized a “divide and conquer” approach in which we first obtained resonance assignments for BamA’s periplasmic POTRA domains 4 and 5 by solution NMR. Comparison of these assignments to solid-state NMR (ssNMR) data obtained on two BamA constructs including the transmembrane domain and one or two soluble POTRA domains suggested that the fold of POTRA domain 5 critically depends on the interface with POTRA 4. Using specific labeling schemes we furthermore obtained ssNMR resonance assignments for residues in the extracellular loop 6 that is known to be crucial for BamA-mediated substrate folding and insertion. Taken together, our data provide novel insights into the conformational stability of membrane-embedded, non-crystalline BamA.
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页码:321 / 332
页数:11
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