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Infectious Complications of Multiple Sclerosis Therapies: Implications for Screening, Prophylaxis, and Management

机译:多发性硬化症疗法的感染性并发症:筛选,预防和管理的含义。

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Multiple sclerosis therapies include interferons, glatiramer, and multiple immunosuppressive drugs. Discerning infectious risks of immunosuppressive drugs requires understanding their mechanisms of action and analyzing interventional studies and postmarketing observational data. Though identical immunosuppressive therapies are sometimes used in non-neurologic conditions, infectious risks may differ in this population. Screening for and treatment of latent tuberculosis (TB) infection should be prioritized for patients receiving alemtuzumab; ocrelizumab is likely not associated with an increased risk of TB. Hepatitis B virus (HBV) reactivation can be devastating for patients treated with ocrelizumab and alemtuzumab, whereas the small molecule oral agents do not likely pose substantial risk of HBV. Progressive multifocal leukoencephalopathy is a particular concern with natalizumab. Alemtuzumab, and possibly natalizumab and fingolimod, risks herpes virus reactivation and may warrant prophylaxis. Unusual opportunistic infections have been described. Vaccination is an important tool in preventing infections, though vaccine timing and contraindications can be complex.
机译:多种硬化症疗法包括干扰素,格拉替雷和多种免疫抑制药物。识别免疫抑制药物的感染风险需要了解其作用机制,并分析干预研究和上市后的观察数据。尽管有时在非神经系统疾病中使用相同的免疫抑制疗法,但该人群的感染风险可能有所不同。对于接受alemtuzumab的患者,应优先筛查和治疗潜伏性结核(TB)感染; ocrelizumab可能与结核病风险增加无关。用ocrelizumab和alemtuzumab治疗的患者乙肝病毒(HBV)的重新活化可能是毁灭性的,而小分子口服药物不太可能带来大量的HBV风险。进行性多灶性白质脑病是那他珠单抗的一项特别关注。 Alemtuzumab,还有那他珠单抗和芬戈莫德,可能会引起疱疹病毒再激活,并可能需要预防。已经描述了不寻常的机会感染。疫苗接种是预防感染的重要工具,尽管疫苗时机和禁忌症可能很复杂。

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