Anti-Mitochondrial Antibodies and Primary Biliary Cirrhosis in TGF-β Receptor II Dominant-Negative Mice

原发性胆汁性肝硬化 自身免疫 分子模拟 生物 免疫学 炎症 T细胞受体 自身免疫性疾病 抗体 细胞因子 转基因小鼠 发病机制 胆汁性肝硬化 转基因 受体 T细胞 免疫系统 基因 遗传学
作者
Sabine Oertelt‐Prigione,Zhe‐Xiong Lian,Chun-Mei Cheng,Ya‐Hui Chuang,Kerstien A. Padgett,Xiaosong He,William M. Ridgway,Aftab A. Ansari,Ross L. Coppel,Ming O. Li,Richard A. Flavell,Mitchell Kronenberg,Lauren Grace Mackey,M. Eric Gershwin
出处
期刊:Journal of Immunology [American Association of Immunologists]
卷期号:177 (3): 1655-1660 被引量:249
标识
DOI:10.4049/jimmunol.177.3.1655
摘要

Primary biliary cirrhosis (PBC) is an autoimmune disease of the liver, characterized by lymphocytic infiltrates in portal tracts, selective destruction of biliary epithelial cells, and anti-mitochondrial Abs (AMAs). The elucidation of early events in the induction of tissue inflammation and autoimmunity in PBC has been hampered by the cryptic onset of the disease, the practical limitations in accessing the target tissue, and the lack of a suitable animal model. We demonstrate in this study that a mouse transgenic for directed expression of a dominant-negative form of TGF-beta receptor type II (dnTGFbetaRII), under the direction of the CD4 promoter, mimics several key phenotypic features of human PBC, including spontaneous production of AMAs directed to the same mitochondrial autoantigens, namely PDC-E2, BCOADC-E2, and OGDC-E2. The murine AMAs also inhibit PDC-E2 activity. Moreover, there is lymphocytic liver infiltration with periportal inflammation analogous to the histological profile in human PBC. Additionally, the serum cytokine profile of affected mice mimics data in human PBC. The concomitant presence of these immunopathological features in the transgenic mice suggests that the TGF-betaRII pathway is implicated in the pathogenesis of PBC. Finally, these data point away from initiation of autoimmunity by mechanisms such as molecular mimicry and more toward activation of an intrinsically self-reactive T cell repertoire in which necessary regulatory T cell influences are lacking.
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