
AbstractThe pathogenic bacterium Salmonella enterica serovar Typhimurium utilizes two type III secretion systems (T3SS) to inject effector proteins into target cells upon infection. The T3SS secretion apparatus (the injectisome) is a large macromolecular assembly composed of over twenty proteins, many in highly oligomeric states. A sub‐structure of the injectisome, termed the basal body, spans both membranes and the periplasmic space of the bacterium. It is primarily composed of three integral membranes proteins, InvG, PrgH, and PrgK, that form ring structures through which components are secreted. In particular, PrgK possesses a periplasmic region consisting of two globular domains joined by a linker polypeptide. We showed previously that in isolation, this region adopts two distinct conformations, of with only one is observed in the assembled basal body complex. Here, using NMR spectroscopy, we further characterize these two conformations. In particular, we demonstrate that the interaction of the linker region with the first globular domain, as found in the intact basal body, is dependent upon the cis conformation of the Leu77‐Pro78 peptide. Furthermore, this interaction is pH‐dependent due to coupling with hydrogen bond formation between Tyr75 and His42 in its neutral Nδ1H tautomeric form. This pH‐dependent interaction may play a role in the regulation of the secretion apparatus disassembly in the context of bacterial infection.
Models, Molecular, 570, Type III Secretion Systems/chemistry, Protein Conformation, Molecular, 500, Salmonella enterica, Hydrogen-Ion Concentration, Models, Type III Secretion Systems, Salmonella enterica/chemistry
Models, Molecular, 570, Type III Secretion Systems/chemistry, Protein Conformation, Molecular, 500, Salmonella enterica, Hydrogen-Ion Concentration, Models, Type III Secretion Systems, Salmonella enterica/chemistry
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