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Update on pathogenesis and treatment of CLE

机译:CLE的发病机理和治疗方法的最新进展

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PURPOSE OF REVIEW: Cutaneous Lupus Erythematous (CLE) is an autoimmune disease in which patients may present with isolated skin findings or have CLE associated with underlying systemic disease. The most significant recent studies on its pathogenesis and therapeutic management are reviewed here. RECENT FINDINGS: Patients with subacute and Discoid Lupus Erythematous had elevated Interferon score, about a third of all cases of SCLE could be attributed to previous drug exposure, and smoking may be more closely associated with CLE than Systemic Lupus Erythematous (SLE). An underlying genetic defect in some subsets of CLE patients may also be shared with SLE. Efficacy of antimalarial therapy is enhanced by increasing treatment duration or maintaining higher blood drug concentrations. Combination antimalarials that include quinacrine, thalidomide analogs, and Mycophenalate Mofetil may also be effective in refractory CLE. SUMMARY: The pathogenesis of CLE remains unclear, and is likely multifactorial. Identified associations with subsets of CLE suggest future research questions in CLE pathogenesis. Subsets of CLE associated with interface dermatitis may share an underlying genetic defect in interferon signaling with SLE. The Cutaneous Lupus Disease Area and Severity Index is a valuable and widely used tool allowing standardized assessment and reporting of cutaneous disease activity and damage. More evidence is available to guide treatment of refractory CLE, but larger studies are needed.
机译:审查目的:皮肤红斑狼疮(CLE)是一种自身免疫性疾病,患者可能表现出孤立的皮肤表现或与潜在的全身性疾病相关的CLE。这里回顾了有关其发病机理和治疗方法的最重要的最新研究。最近的发现:亚急性和盘状红斑狼疮患者的干扰素评分升高,所有SCLE病例中约有三分之一可归因于以前的药物暴露,吸烟与CLE的关系可能比全身性红斑狼疮(SLE)更为密切。 SLE也可能共享一些CLE患者亚型的潜在遗传缺陷。通过延长治疗时间或维持较高的血液药物浓度,可以提高抗疟疾治疗的功效。包括奎纳克林,沙利度胺类似物和Mycophenalate Mofetil的组合抗疟药也可能在难治性CLE中有效。摘要:CLE的发病机制仍不清楚,可能是多因素的。与CLE子集相关的关联提示了CLE发病机理的未来研究问题。与界面皮炎相关的CLE亚型可能与SLE的干扰素信号传导共享潜在的遗传缺陷。皮肤狼疮疾病面积和严重性指数是一种有价值的且被广泛使用的工具,可以对皮肤疾病的活动和损害进行标准化评估和报告。有更多证据可指导难治性CLE的治疗,但还需要进行更大的研究。

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