新生儿去胸腺小鼠免疫介导胆管肝炎的诱导和持续

Toshiyuki Masanaga , Yasuyuki Watanabe , Judy Van de Water , Patrick S.C. Leung , Toshio Nakanishi , Goro Kajiyama , Boris H. Ruebner , Ross L. Coppel , M.Eric Gershwin
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引用次数: 20

摘要

重组自身抗原的可用性使得原发性胆汁性肝硬化(PBC)和线粒体抗原之间关系的实验研究成为可能。我们利用这些重组自身抗原,并试图通过免疫新生胸腺切除(NTx)脂多糖(LPS)处理的A/J小鼠来诱导自身免疫性胆管炎,已知这些小鼠容易发生器官特异性自身免疫性疾病。我们使用了一种含有双头分子的重组蛋白,该分子共表达丙酮酸脱氢酶复合物和支链酮酸脱氢酶复合物E2亚基的免疫优势表位。我们在此报道,通过这种免疫和同时注射LPS诱导NTx小鼠免疫介导的胆管肝炎。胆管炎的发生率在NTx,免疫,LPS组为79%,而在NTx,未免疫,LPS组为14%。组织病理学从轻度到重度不等,包括胆管损伤、局灶性肝坏死和内皮炎,但无肉芽肿。此外,在停止免疫和LPS注射后,NTx小鼠几乎所有这些病变都持续了12周。有趣的是,我们成功地(89%)将NTx免疫LPS小鼠的肝脏浸润性单核细胞移植到先天性未免疫的NTx小鼠中;这种病变不能随脾细胞转移。虽然病理不是典型的PBC,但该模型为研究免疫介导的肝胆损伤提供了独特的场所。
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Induction and Persistence of Immune-Mediated Cholangiohepatitis in Neonatally Thymectomized Mice

The availability of recombinant autoantigens allows the experimental study of the relationships between primary biliary cirrhosis (PBC) and mitochondrial antigens. We took advantage of these recombinant autoantigens and attempted to induce autoimmune cholangitis by immunizing neonatally thymectomized (NTx) lipopolysaccharide (LPS)-treated A/J mice, known to be prone to organ-specific autoimmune diseases. We employed a recombinant protein containing a dual-headed molecule that coexpresses the immunodominant epitope of the E2 subunits of the pyruvate dehydrogenase complex and the branched-chain keto-acid dehydrogenase complex. We report herein that an immune-mediated cholangiohepatitis was induced by such immunization and the concurrent injection of LPS into NTx mice. The incidence of cholangitis was 79% in the NTx, immunized, LPS group compared to 14% in the NTx, nonimmunized, LPS group. The histopathology ranged from mild to severe and included bile duct damage, focal hepatic necrosis, and endotheliitis, but no granulomas. Moreover, almost all such lesions persisted for 12 weeks after the discontinuation of immunization and LPS injections in the NTx mice. Interestingly, we were successful (89%) in transferring the cholangiohepatitis by injection of liver infiltrating mononuclear cells from the NTx, immunized, LPS mice into congenic nonimmunized NTx mice; such lesions could not be transferred with spleen cells. Although the pathology is not typical of PBC, this model offers a unique venue for the study of immune-mediated hepatobiliary injury.

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