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Autoimmune liver disease.

机译:自身免疫性肝病。

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摘要

PURPOSE OF REVIEW: To review studies that improve the diagnosis and treatment of autoimmune hepatitis and extend understanding of its pathogenic mechanisms. RECENT FINDINGS: Black patients have more advanced disease and poorer outcomes than white patients. Genome-wide DNA microsatellite techniques have identified multiple regions that may confer susceptibility or resistance to the disease. Preferential inactivation of one parentally-derived X chromosome may favor autoreactivity in women. Acute and chronic hepatitis of undetermined cause can respond to corticosteroid therapy and represent autoantibody-negative autoimmune hepatitis. Outcomes can be improved by continuing therapies until resolution of all features and by early identification of problematic patients with the Model for End Stage Liver Disease. Serum levels of B-cell activating factor correlate with laboratory indices of liver injury. Tacrolimus and mycophenolate mofetil are promising therapies for problematic patients, and the antigenic targets of atypical antibodies to liver/kidney microsome may lead to diagnostic tests for de-novo autoimmune hepatitis after liver transplantation. SUMMARY: Ethnic background and genetic predisposition affect the occurrence and outcome of autoimmune hepatitis. Susceptibility and resistance factors across the human genome underscore the genetic complexity of the disease. Outcomes can be improved by better use of current regimens and further evaluation of action-specific immunosuppressive agents.
机译:审查目的:审查可改善自身免疫性肝炎的诊断和治疗并扩大其致病机理的研究。最新发现:黑人患者比白人患者病情更严重,预后较差。全基因组DNA微卫星技术已鉴定出多个区域,可能赋予该病易感性或抗性。优先灭活一个父母衍生的X染色体可能有助于女性自身反应。病因不明的急性和慢性肝炎可对皮质类固醇激素疗法产生反应,代表自身抗体阴性的自身免疫性肝炎。通过持续治疗直至所有特征得到解决,以及通过尽早发现患有晚期肝病模型的有问题的患者,可以改善结果。血清B细胞活化因子水平与肝脏损伤的实验室指标相关。他克莫司和霉酚酸酯是有问题的患者的有前途的治疗方法,肝/肾微粒体的非典型抗体的抗原性靶点可能会导致肝移植后新型自身免疫性肝炎的诊断测试。摘要:种族背景和遗传易感性影响自身免疫性肝炎的发生和结局。整个人类基因组中的易感性和耐药性因素强调了该疾病的遗传复杂性。可以通过更好地使用当前方案和进一步评估特定于动作的免疫抑制剂来改善结果。

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