Factor B as a therapeutic target for the treatment of complement-mediated diseases

补体系统 替代补体途径 补体因子B 伊库利珠单抗 免疫学 经典补体途径 补体膜攻击复合物 非典型溶血尿毒综合征 凝集素途径 阵发性夜间血红蛋白尿 补体成分2 C3转化酶 补体因子I 医学 生物 抗体
作者
David Kavanagh,Jonathan Barratt,Anna Schubart,Nicholas J.A. Webb,Matthias Meier,Fádi Fakhouri
出处
期刊:Frontiers in Immunology [Frontiers Media]
卷期号:16: 1537974-1537974 被引量:14
标识
DOI:10.3389/fimmu.2025.1537974
摘要

The complement system, consisting of three initiating pathways-classical, lectin and alternative, is an important part of innate immunity. Dysregulation of the complement system is implicated in the pathogenesis of several autoimmune and inflammatory diseases. Therapeutic inhibition of the complement system has been recognized as a viable approach to drug development and has been successful with the approval of a small number of complement inhibitors for diseases such as paroxysmal nocturnal hemoglobinuria, atypical hemolytic uremic syndrome, neuromyelitis optica, myasthenia gravis and geographic atrophy. More recently, therapies selectively targeting the alternative pathway (AP), which drives the amplification of the complement responses, are being evaluated for these complement-mediated diseases. Complement Factor B, a serine protease, is a unique component of the AP that is essential for the catalytic activity of AP C3 convertase and AP C5 convertase. Inhibition of Factor B blocks the activity of the alternative pathway and the amplification loop, and subsequent generation of the membrane attack complex downstream; however, it has no effect on the initial activation mediated by the classical and lectin complement pathways. Therefore, Factor B is an attractive target for diseases in which the AP is overactivated. In this review, we provide an overview of Factor B and its critical role in the AP, discuss the benefit-risk of Factor B inhibition as a targeted therapeutic strategy, and describe the various Factor B inhibitors that are approved and/or in clinical development.
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