FcRn Inhibitor Therapies in Neurologic Diseases.

IF 7.4 2区医学 Q1 CLINICAL NEUROLOGY CNS drugs Pub Date : 2024-06-01 Epub Date: 2024-05-09 DOI:10.1007/s40263-024-01090-3

Nouf Alfaidi, Salama Karmastaji, Alexandria Matic, Vera Bril

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Abstract

In the last decade, the landscape of treating autoimmune diseases has evolved with the emergence and approval of novel targeted therapies. Several new biological agents offer selective and target-specific immunotherapy and therefore fewer side effects, such as neonatal Fc receptor (FcRn)-targeting therapy. Neonatal Fc receptor-targeted therapies are engineered to selectively target FcRn through various methods, such as Fc fragments or monoclonal anti-FcRn antibodies. These approaches enhance the breakdown of autoantibodies by blocking the immunoglobulin G recycling pathway. This mechanism reduces overall plasma immunoglobulin levels, including the levels of pathogenic autoantibodies, without affecting the other immunoglobulin class immunoglobulin A, immunoglobulin E, immunoglobulin M, and immunoglobulin D levels. Drugs that inhibit FcRn include efgartigimod, rozanolixizumab, batoclimab, and nipocalimab. These medications can be administered either intravenously or subcutaneously. Numerous clinical trials are currently underway to investigate their effectiveness, safety, and tolerability in various neurological conditions, including myasthenia gravis and other neurological disorders such as chronic inflammatory demyelinating polyneuropathy, myositis, neuromyelitis optica, and myelin oligodendrocyte glycoprotein antibody disease. Positive results from clinical trials of efgartigimod and rozanolixizumab led to their approval for the treatment of generalized myasthenia gravis. Additional clinical trials are still ongoing. Neonatal Fc receptor inhibitor agents seem to be well tolerated. Reported adverse events include headache (most commonly observed with efgartigimod and rozanolixizumab), upper respiratory tract infection, urinary tract infection, diarrhea, pyrexia, and nausea. Additionally, some of these agents may cause transient hypoalbuminemia and hypercholesterolemia notably reported with batoclimab and nipocalimab. In this review, we discuss the available clinical data for FcRN inhibitor agents in treating different neurological autoimmune diseases.

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神经系统疾病中的 FcRn 抑制剂疗法。

近十年来，随着新型靶向疗法的出现和获批，治疗自身免疫性疾病的格局发生了变化。一些新型生物制剂提供了选择性和靶向特异性免疫疗法，因此副作用较少，例如新生儿 Fc 受体（FcRn）靶向疗法。新生儿 Fc 受体靶向疗法通过各种方法，如 Fc 片段或单克隆抗 FcRn 抗体，选择性地靶向 FcRn。这些方法通过阻断免疫球蛋白 G 的循环途径来加强自身抗体的分解。这种机制可降低血浆免疫球蛋白的总体水平，包括致病性自身抗体的水平，而不会影响其他免疫球蛋白类免疫球蛋白 A、免疫球蛋白 E、免疫球蛋白 M 和免疫球蛋白 D 的水平。抑制 FcRn 的药物包括依加替莫德（efgartigimod）、罗扎尼珠单抗（rozanolixizumab）、巴妥珠单抗（batoclimab）和尼泊卡单抗（nipocalimab）。这些药物可以静脉注射或皮下注射。目前正在进行大量临床试验，以研究这些药物对各种神经系统疾病的有效性、安全性和耐受性，包括重症肌无力和其他神经系统疾病，如慢性炎症性脱髓鞘性多发性神经病、肌炎、神经性视脊髓炎和髓鞘少突胶质细胞糖蛋白抗体病。依加替莫德（efgartigimod）和罗扎尼珠单抗（rozanolixizumab）的临床试验结果良好，因此被批准用于治疗全身性重症肌无力。其他临床试验仍在进行中。新生儿 Fc 受体抑制剂似乎耐受性良好。已报告的不良反应包括头痛（最常见于依加替莫德和罗扎尼单抗）、上呼吸道感染、泌尿道感染、腹泻、发热和恶心。此外，这些药物中的一些可能会导致一过性低白蛋白血症和高胆固醇血症，巴妥珠单抗和尼泊卡珠单抗的报道尤为明显。在本综述中，我们将讨论 FcRN 抑制剂治疗不同神经系统自身免疫性疾病的现有临床数据。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

CNS drugs 医学-精神病学

CiteScore

12.00

自引率

3.30%

发文量

审稿时长

6-12 weeks

期刊介绍： CNS Drugs promotes rational pharmacotherapy within the disciplines of clinical psychiatry and neurology. The Journal includes: - Overviews of contentious or emerging issues. - Comprehensive narrative reviews that provide an authoritative source of information on pharmacological approaches to managing neurological and psychiatric illnesses. - Systematic reviews that collate empirical evidence to answer a specific research question, using explicit, systematic methods as outlined by the PRISMA statement. - Adis Drug Reviews of the properties and place in therapy of both newer and established drugs in neurology and psychiatry. - Original research articles reporting the results of well-designed studies with a strong link to clinical practice, such as clinical pharmacodynamic and pharmacokinetic studies, clinical trials, meta-analyses, outcomes research, and pharmacoeconomic and pharmacoepidemiological studies. Additional digital features (including animated abstracts, video abstracts, slide decks, audio slides, instructional videos, infographics, podcasts and animations) can be published with articles; these are designed to increase the visibility, readership and educational value of the journal’s content. In addition, articles published in CNS Drugs may be accompanied by plain language summaries to assist readers who have some knowledge of, but not in-depth expertise in, the area to understand important medical advances.