在主要组织相容性复合体II类缺陷的MRL-lpr小鼠中预防肾炎
Prevention of nephritis in major histocompatibility complex class II-deficient MRL-lpr mice.
作者信息
Jevnikar A M, Grusby M J, Glimcher L H
机构信息
Robarts Research Institute, University of Western Ontario, London, Canada.
出版信息
J Exp Med. 1994 Apr 1;179(4):1137-43. doi: 10.1084/jem.179.4.1137.
Abstract
MRL-lpr mice develop aggressive autoimmune kidney disease associated with increased or de novo renal expression of major histocompatibility complex (MHC) class II molecules and a massive systemic expansion of CD4-CD- double negative (DN) T cells. Whereas non-MHC linked genes can have a profound effect on the development of nephritis, lymphadenopathy, and anti-DNA antibody production in MRL-lpr mice, the role of MHC molecules has not been unequivocally established. To study the role of MHC class II in this murine model of systemic lupus erythematosis, class II-deficient MRL-lpr mice (MRL-lpr -/-) were created. MRL-lpr -/- mice developed lymphadenopathy but not autoimmune renal disease or autoantibodies. This study demonstrates that class II expression is critical for the development of autoaggressive CD4+ T cells involved in autoimmune nephritis and clearly dissociates DN T cell expansion from autoimmune disease initiation.
摘要
MRL-lpr小鼠会发展出侵袭性自身免疫性肾病,这与主要组织相容性复合体(MHC)II类分子在肾脏中的表达增加或从头表达以及CD4-CD-双阴性(DN)T细胞的大量系统性扩增有关。虽然非MHC连锁基因可对MRL-lpr小鼠的肾炎、淋巴结病和抗DNA抗体产生的发展产生深远影响,但MHC分子的作用尚未得到明确证实。为了研究MHC II类分子在这种系统性红斑狼疮小鼠模型中的作用,构建了II类缺陷型MRL-lpr小鼠(MRL-lpr -/-)。MRL-lpr -/-小鼠出现了淋巴结病,但未出现自身免疫性肾病或自身抗体。这项研究表明,II类分子的表达对于参与自身免疫性肾炎的自身攻击性CD4+ T细胞的发育至关重要,并且清楚地将DN T细胞扩增与自身免疫性疾病的起始区分开来。
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