【 摘 要 】

Moststaphylococciproduceshortα‐typePSMsandabouttwiceaslongβ‐typePSMsthatarepotentleukocyteattractantsandtoxins.PSMsareusuallysecretedwiththeN‐terminalformylgroupbutareonlyweakagonistsfortheleukocyteFPR1.Instead,theFPR1‐relatedFPR2sensesPSMsefficientlyandiscrucialforleukocyterecruitmentininfection.WhichstructuralfeaturesdistinguishFPR1fromFPR2ligandshasremainedelusive.Toanalyzewhichpeptidepropertiesmaygovernthecapacitiesofβ‐typePSMstoactivateFPRs,full‐lengthandtruncatedvariantsofsuchpeptidesfromStaphylococcusaureus,Staphylococcusepidermidis,andStaphylococcuslugdunensisweresynthesized.FPR2activationwasobservedevenforshortN‐orC‐terminalβ‐typePSMvariantsoncetheywerelongerthan18aa,andthisactivityincreasedwithlength.Incontrast,theshortesttestedpeptideswerepotentFPR1agonists,andthispropertydeclinedwithincreasingpeptidelength.Whereasfull‐lengthβ‐typePSMsformedα‐helicesandexhibitednoFPR1‐specificactivity,thetruncatedpeptideshadless‐stablesecondarystructures,wereweakagonistsforFPR1,andrequiredN‐terminalformyl‐methionineresiduestobeFPR2agonists.Together,thesedatasuggestthatFPR1andFPR2haveopposedligandpreferences.Short,flexiblePSMstructuresmayfavorFPR1butnotFPR2activation,whereaslongerpeptideswithα‐helical,amphipathicpropertiesarestrongFPR2butonlyweakFPR1agonists.Thesefindingsshouldhelptounraveltheligandspecificitiesof2criticalhumanPRRs,andtheymaybeimportantfornew,anti‐infectiveandanti‐inflammatorystrategies...

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