【 摘 要 】

Theimmunologicalsynapseisahighlystructuredandmolecularlydynamicinterfacebetweencommunicatingimmunecells.AlthoughtheimmunologicalsynapsepromotesTcellactivationbydendriticcells,thespecificorganizationoftheimmunologicalsynapseonthedendriticcellsideinresponsetoTcellengagementislargelyunknown.Inthisstudy,confocalandelectronmicroscopytechniqueswereusedtoinvestigatetheroleofdendriticcellactinregulationinimmunologicalsynapseformation,stabilization,andfunction.Inthedendriticcell‐restrictedabsenceoftheWiskott‐Aldrichsyndromeprotein,animportantregulatoroftheactincytoskeletoninhematopoieticcells,theimmunologicalsynapsecontactwithTcellsoccupiedasignificantlyreducedsurfacearea.Atamolecularlevel,theactinnetworklocalizedtotheimmunologicalsynapseexhibitedreducedstability,inparticular,oftheactin‐relatedprotein‐2/3‐dependent,short‐filamentnetwork.Thiswasassociatedwithdecreasedpolarizationofdendriticcell‐associatedICAM‐1andMHCclassII,whichwaspartiallydependentonWiskott‐Aldrichsyndromeproteinphosphorylation.Withtheuseofsupportedplanarlipidbilayersincorporatinganti‐ICAM‐1andanti‐MHCclassIIantibodies,thedendriticcellactincytoskeletonorganizedintorecognizablesynapticstructuresbutinterestingly,formedWiskott‐Aldrichsyndromeprotein‐dependentpodosomeswithinthisarea.Thesefindingsdemonstratethatintrinsicdendriticcellcytoskeletalremodelingisakeyregulatorycomponentofnormalimmunologicalsynapseformation,likelythroughconsolidationofadhesiveinteractionandmodulationofimmunologicalsynapsestability...

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