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Protection from EAE in DOCK8 mutant mice occurs despite increased Th17 cell frequencies in the periphery

dc.contributor.authorWilson, Alicia
dc.contributor.authorLaw, Hsei Di
dc.contributor.authorKnobbe-Thomsen, Christiane B
dc.contributor.authorKearney, Connor J
dc.contributor.authorOliaro, Jane
dc.contributor.authorBinsfeld, Carole
dc.contributor.authorBurgio, Gaetan
dc.contributor.authorStarrs, Lora
dc.contributor.authorBrenner, Dirk
dc.contributor.authorRandall, Katrina
dc.contributor.authorBruestle, Anne
dc.date.accessioned2023-01-13T01:03:50Z
dc.date.issued2019
dc.date.updated2021-11-28T07:35:19Z
dc.description.abstractMutation of Dedicator of cytokinesis 8 (DOCK8) has previously been reported to provide resistance to the Th17 cell dependent EAE in mice. Contrary to expectation, we observed an elevation of Th17 cells in two different DOCK8 mutant mouse strains in the steady state. This was specific for Th17 cells with no change in Th1 or Th2 cell populations. In vitro Th cell differentiation assays revealed that the elevated Th17 cell population was not due to a T cell intrinsic differentiation bias. Challenging these mutant mice in the EAE model, we confirmed a resistance to this autoimmune disease with Th17 cells remaining elevated systemically while cellular infiltration in the CNS was reduced. Infiltrating T cells lost the bias toward Th17 cells indicating a relative reduction of Th17 cells in the CNS and a Th17 cell specific migration disadvantage. Adoptive transfers of Th1 and Th17 cells in EAE‐affected mice further supported the Th17 cell‐specific migration defect, however, DOCK8‐deficient Th17 cells expressed normal Th17 cell‐specific CCR6 levels and migrated toward chemokine gradients in transwell assays. This study shows that resistance to EAE in DOCK8 mutant mice is achieved despite a systemic Th17 bias.en_AU
dc.description.sponsorshipThis work was supported by an Australian Government Research Training Program Scholarship (A.S.W.), NHMRC project grants 1022922 (K.L.R.) and 1079318 (J.O., K.L.R.), ACT Health Private Practice Fund Major Grant 2015 and 2016 (K.L.R). C.B.K.T. was supported by the DKH (110663) and the BMBF (01ZX1401B). D.B. is funded through the FNR-ATTRACT program (A14/BM/7632103) and an FNR-CORE grant (C15/BM/10355103) of the Luxembourg National Research Fund. The authors thank all members of the Brüstle laboratory, past and present, for their support and the flow cytometry facility at The John Curtin School of Medical Research for their excellent services. The authors further thank Dr. Emmalene Bartlett for her insightful scientific editing.en_AU
dc.format.mimetypeapplication/pdfen_AU
dc.identifier.issn0014-2980en_AU
dc.identifier.urihttp://hdl.handle.net/1885/282743
dc.language.isoen_AUen_AU
dc.publisherWiley-VCH Verlag GMBHen_AU
dc.relationhttp://purl.org/au-research/grants/nhmrc/1022922en_AU
dc.relationhttp://purl.org/au-research/grants/nhmrc/1079318en_AU
dc.sourceEuropean Journal of Immunologyen_AU
dc.subjectCD4 T cellsen_AU
dc.subjectdedicator of Cytokinesis 8en_AU
dc.subjectexperimental autoimmune encephalomyeli-tisen_AU
dc.subjectmigrationen_AU
dc.subjectTh17 cellsen_AU
dc.titleProtection from EAE in DOCK8 mutant mice occurs despite increased Th17 cell frequencies in the peripheryen_AU
dc.typeJournal articleen_AU
local.bibliographicCitation.issue5en_AU
local.bibliographicCitation.lastpage781en_AU
local.bibliographicCitation.startpage770en_AU
local.contributor.affiliationWilson, Alicia, College of Health and Medicine, ANUen_AU
local.contributor.affiliationLaw, Hsei Di, College of Health and Medicine, ANUen_AU
local.contributor.affiliationKnobbe-Thomsen, Christiane B, Heinrich Heine Universityen_AU
local.contributor.affiliationKearney, Connor J, Peter MacCallum Caner Centreen_AU
local.contributor.affiliationOliaro, Jane, Peter MacCallum Cancer Centreen_AU
local.contributor.affiliationBinsfeld, Carole, Luxembourg Institute of Healthen_AU
local.contributor.affiliationBurgio, Gaetan, College of Health and Medicine, ANUen_AU
local.contributor.affiliationStarrs, Lora, College of Health and Medicine, ANUen_AU
local.contributor.affiliationBrenner, Dirk, Luxembourg Institute of Healthen_AU
local.contributor.affiliationRandall, Katrina, College of Health and Medicine, ANUen_AU
local.contributor.affiliationBruestle, Anne, College of Health and Medicine, ANUen_AU
local.contributor.authoruidWilson, Alicia, u5007341en_AU
local.contributor.authoruidLaw, Hsei Di, u4469589en_AU
local.contributor.authoruidBurgio, Gaetan, u5727247en_AU
local.contributor.authoruidStarrs, Lora, u4301798en_AU
local.contributor.authoruidRandall, Katrina, u4259040en_AU
local.contributor.authoruidBruestle, Anne, u5691124en_AU
local.description.embargo2099-12-31
local.description.notesImported from ARIESen_AU
local.identifier.absfor320404 - Cellular immunologyen_AU
local.identifier.absfor320906 - Peripheral nervous systemen_AU
local.identifier.absseo280103 - Expanding knowledge in the biomedical and clinical sciencesen_AU
local.identifier.absseo200105 - Treatment of human diseases and conditionsen_AU
local.identifier.ariespublicationu5786633xPUB766en_AU
local.identifier.citationvolume49en_AU
local.identifier.doi10.1002/eji.201847960en_AU
local.identifier.scopusID2-s2.0-85061803808
local.publisher.urlhttps://onlinelibrary.wiley.com/en_AU
local.type.statusPublished Versionen_AU

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