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Current concepts in the diagnosis, pathogenesis, and treatment of autoimmune hepatitis.

机译:自身免疫性肝炎的诊断,发病机制和治疗中的当前概念。

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摘要

Autoimmune hepatitis has a global distribution and affects all ages. Genetic factors strongly influence susceptibility, clinical expression, and treatment response. The diagnosis of autoimmune hepatitis has been codified by an international panel. An acute or fulminant presentation is recognized but not a cholestatic form. Subclassifications by predominant autoantibody profile have been proposed, but they lack etiologic and prognostic differences. Autoantibodies continue to be characterized to improve diagnostic specificity, predict outcome, and identify pertinent antigenic targets. Cytosolic enzymes are prime candidates as autoantigens. DRB1*0301 and DRB1*0401 are the susceptibility alleles in Caucasoid Northern Europeans and North Americans, and they also affect clinical expression and treatment outcome. Other autoimmune promoters affecting cytokine production and immunocyte activation may act in synergy with the susceptibility alleles to affect disease behavior. Cell-mediated and antibody-dependent forms of cytotoxicity are probably interactive pathogenic mechanisms, and novel site-specific therapies are feasible because these mechanisms are defined. Potent new immunosuppressive agents are emerging from the transplantation arena, but prednisone alone or in combination with azathioprine remains the mainstay of treatment. Corticosteroid therapy is effective but not ideal.
机译:自身免疫性肝炎分布全球,并影响各个年龄段。遗传因素强烈影响药敏性,临床表达和治疗反应。国际专家小组已对自身免疫性肝炎的诊断进行了整理。可以识别为急性或暴发性表现,但不能呈胆汁淤积形式。已经提出了以主要自身抗体谱为基础的亚类,但它们缺乏病因学和预后差异。自身抗体继续被表征为改善诊断特异性,预测结果并鉴定相关抗原靶标。胞溶酶是自身抗原的主要候选物。 DRB1 * 0301和DRB1 * 0401是在高加索地区的北欧人和北美人中的易感性等位基因,它们也影响临床表达和治疗效果。其他影响细胞因子产生和免疫细胞活化的自身免疫启动子可能与易感性等位基因协同作用,从而影响疾病行为。细胞介导的和抗体依赖性的细胞毒性形式可能是相互作用的致病机制,新的位点特异性疗法是可行的,因为已定义了这些机制。强有力的新型免疫抑制剂正在移植领域兴起,但泼尼松单独或与硫唑嘌呤联用仍是治疗的主要手段。皮质类固醇激素疗法有效,但不理想。

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