Optimizing chronic inflammatory demyelinating polyneuropathy care with subcutaneous immunoglobulin: The Polyneuropathy and Treatment with Hizentra Open-Label Extension (PATH OLE) study and beyond

Mazen M. Dimachkie
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Abstract

Chronic inflammatory demyelinating polyneuropathy (CIDP) is a heterogeneous, acquired autoimmune neurological disorder affecting peripheral nerves. CIDP is characterized by progressive weakness, reduced or absent tendon reflexes and impaired sensory function in the lower and upper limbs. CIDP diagnosis is mainly based on clinical, laboratory and electrophysiologic criteria and there are currently no diagnostic or prognostic biomarkers. First-line treatment options include corticosteroids, intravenous immunoglobulin (IVIg) and plasma exchange (PLEX). While IVIg and corticosteroids are the most common therapies administered for CIDP, there are challenges associated with their use, including systemic adverse events (AEs), some of which can be serious. Studies have shown that subcutaneous immunoglobulin (SCIg) may be associated with improved quality of life, which is attributed partially to the patients’ freedom to administer SCIg at home and at their convenience. While AEs with SCIg mostly consist of local site reactions, SCIg is associated with fewer systemic AEs compared with IVIg, and these are commonly mild, though severe reactions may rarely occur. A number of studies in the last decade have assessed SCIg in CIDP. One of these studies, the Polyneuropathy and Treatment with Hizentra® (PATH) study, was a global phase 3, double-blind, randomized, placebo-controlled trial that assessed the efficacy, safety, and tolerability of SCIg treatment in patients with CIDP. Based on the results of the PATH study, the US Food and Drug Administration (FDA) approved SCIg as a maintenance treatment for CIDP in 2018. This review summarizes and discusses the results of the PATH study and its open-label extension (OLE) study and provides an overview of the April 2021 update to the Hizentra® FDA-approved U.S. package insert based on findings from the PATH OLE. In addition, the review highlights key elements of the second revision of the European Academy of Neurology/Peripheral Nerve Society (EAN/PNS) guideline for the diagnosis and treatment of CIDP. Finally, this review discusses the characteristics of patients with CIDP who may benefit from SCIg treatment.
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皮下免疫球蛋白优化慢性炎症性脱髓鞘性多神经病变的护理:多神经病变和治疗的Hizentra开放标签扩展(PATH OLE)研究及以后
慢性炎症性脱髓鞘性多神经病变(CIDP)是一种影响周围神经的异质、获得性自身免疫性神经疾病。CIDP的特征是进行性无力,下肢和上肢肌腱反射减少或缺失,感觉功能受损。CIDP的诊断主要基于临床、实验室和电生理标准,目前没有诊断或预后的生物标志物。一线治疗方案包括皮质类固醇、静脉注射免疫球蛋白(IVIg)和血浆置换(PLEX)。虽然IVIg和皮质类固醇是CIDP最常用的治疗方法,但它们的使用存在挑战,包括系统性不良事件(ae),其中一些可能很严重。研究表明,皮下免疫球蛋白(SCIg)可能与生活质量的改善有关,部分原因是患者可以自由地在家中和方便地使用SCIg。虽然SCIg的不良反应主要由局部反应组成,但与IVIg相比,SCIg与更少的系统性不良反应相关,这些不良反应通常是轻微的,尽管严重的反应可能很少发生。在过去十年中,许多研究评估了CIDP中的SCIg。其中一项研究,多神经病变和治疗与Hizentra®(PATH)研究,是一项全球3期,双盲,随机,安慰剂对照试验,评估SCIg治疗CIDP患者的疗效,安全性和耐受性。基于PATH研究的结果,美国食品和药物管理局(FDA)于2018年批准SCIg作为CIDP的维持治疗。本综述总结并讨论了PATH研究及其开放标签扩展(OLE)研究的结果,并概述了基于PATH OLE研究结果的2021年4月fda批准的Hizentra®美国包装说明书更新。此外,该综述还强调了欧洲神经病学学会/周围神经学会(EAN/PNS)诊断和治疗CIDP指南第二版的关键要素。最后,本综述讨论了可能受益于SCIg治疗的CIDP患者的特征。
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