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眼肌型重症肌无力:一个难以捉摸的靶点的最新进展。

Ocular myasthenia gravis: updates on an elusive target.

机构信息

Department of Ophthalmology, University of Oklahoma, Oklahoma City, Oklahoma.

Department of Ophthalmology and Visual Neurosciences, University of Minnesota, Minneapolis, Minnesota, USA.

出版信息

Curr Opin Neurol. 2020 Feb;33(1):55-61. doi: 10.1097/WCO.0000000000000775.

Abstract

PURPOSE OF REVIEW

Ocular myasthenia gravis (OMG) is a complex condition with heterogenous phenotypes and ill-defined diagnostic criteria. Understanding concomitant risk factors and autoimmune serology can help inform prognosis for generalization and guide treatment.

RECENT FINDINGS

Although antibodies to acetylcholine receptors or muscle-specific kinase likely increase risk of generalization, they are less frequent in OMG. Patients without either antibody tend to have a milder disease process and often have variable antibodies to other end-plate proteins such as LRP4, agrin, or cortactin. The treatment of OMG begins with pyridostigmine and is supplemented by oral prednisone if treatment-resistant or high risk for generalization. Variable oral prednisone regimens have been used with success and further immunosuppression may be best achieved with mycophenolate mofetil and azathioprine. Checkpoint inhibitor-induced myasthenia gravis is increasingly recognized and likely has high rates of mortality associated with myocarditis.

SUMMARY

Our understanding of OMG and its variable phenotypes continues to evolve. Autoantibody testing increasingly provides valuable diagnostic and prognostic information. Despite these improvements, a lack of quality treatment trials creates significant challenges for evidence-based management guidelines.

摘要

目的综述

眼肌型重症肌无力(OMG)是一种表现型多样、诊断标准不明确的复杂疾病。了解并存的危险因素和自身免疫性血清学可以帮助预测疾病的泛化,并指导治疗。

最近的发现

尽管乙酰胆碱受体抗体或肌肉特异性激酶抗体可能会增加泛化的风险,但在 OMG 中它们并不常见。没有这些抗体的患者往往疾病过程较轻,并且经常具有其他终板蛋白的可变抗体,如 LRP4、神经节苷脂或桩蛋白。OMG 的治疗始于吡啶斯的明,如果治疗抵抗或有泛化高风险,则用口服泼尼松补充治疗。可变口服泼尼松方案已成功应用,进一步的免疫抑制可能最好通过吗替麦考酚酯和硫唑嘌呤来实现。检查点抑制剂诱导的重症肌无力越来越受到关注,并且可能与心肌炎相关的死亡率很高。

总结

我们对 OMG 及其可变表型的认识仍在不断发展。自身抗体检测越来越多地提供有价值的诊断和预后信息。尽管有这些改进,但缺乏高质量的治疗试验为基于证据的管理指南带来了重大挑战。

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