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首页> 外文期刊>American Journal of Transplantation >Th17 Cells Induce a Distinct Graft Rejection Response That Does Not Require IL-17A
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Th17 Cells Induce a Distinct Graft Rejection Response That Does Not Require IL-17A

机译:Th17细胞诱导不同的移植物排斥反应,不需要IL-17A

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IL-17A-producing helper T (Th17) cells have been implicated in the pathogenesis of autoimmune disease, inflammatory bowel disease and graft rejection, however the mechanisms by which they cause tissue damage remain ill-defined. We examined what damage Th17 cell lines could inflict on allogeneic skin grafts in the absence of other adaptive lymphocytes. CD4+ Th17 cell lines were generated from two TCR transgenic mouse strains, A1(M).RAG1?/? and Marilyn, each monospecific for the male antigen Dby. After prolonged in vitro culture in polarizing conditions, Th17 lines produced high levels of IL-17A with inherently variable levels of interferon gamma (IFN) and these cells were able to maintain IL-17A expression following adoptive transfer into lymphopenic mice. When transferred into lymphopenic recipients of male skin grafts, Th17 lines elicited a damaging reaction within the graft associated with pathological findings of epidermal hyperplasia and neutrophil infiltration. Th17 cells could be found in the grafted skins and spleens of recipients and maintained their polarized phenotype both in vivo and after ex vivo restimulation. Antibody-mediated neutralization of IL-17A or IFN did not interfere with Th17-induced pathology, nor did it prevent neutrophil infiltration. In conclusion, tissue damage by Th17 cells does not require IL-17A.
机译:产生IL-17A的辅助性T(Th17)细胞与自身免疫性疾病,炎性肠病和移植排斥反应的发病机制有关,但是它们引起组织损伤的机制仍不清楚。我们检查了在没有其他适应性淋巴细胞的情况下,Th17细胞系会对同种异体皮肤移植造成何种损害。 CD4 + Th17细胞系由两种TCR转基因小鼠品系A1(M).RAG1 ?/?和Marilyn产生,它们分别对男性抗原Dby具有单特异性。在极化条件下延长体外培养后,Th17细胞系产生高水平的IL-17A,内在干扰素γ(IFN)的水平却发生了变化,这些细胞在过继转移入淋巴细胞减少小鼠后能够维持IL-17A的表达。当转移到雄性皮肤移植物的淋巴细胞减少受体中时,Th17细胞系引起移植物中的损伤反应,并伴随表皮增生和中性粒细胞浸润的病理学发现。 Th17细胞可以在受体的移植皮肤和脾脏中发现,并在体内和离体再刺激后均保持其极化表型。抗体介导的IL-17A或IFN的中和作用不会干扰Th17诱导的病理,也不会阻止中性粒细胞浸润。总之,Th17细胞对组织的损伤不需要IL-17A。

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