新生儿 Fc 受体和 IgG 类治疗药物。
Neonatal Fc receptor and IgG-based therapeutics.
机构信息
Division of Gastroenterology, Department of Medicine, Brigham & Women's Hospital, Harvard Medical School, Boston, MA, USA.
出版信息
MAbs. 2011 Sep-Oct;3(5):422-30. doi: 10.4161/mabs.3.5.16983. Epub 2011 Sep 1.
Abstract
The majority of potent new biologics today are IgG-based molecules that have demonstrated tissue-targeting specificity with favorable clinical response. Several factors determine the efficacy of these products, including target specificity, serum half-life and effector functions via complement-dependent cytotoxicity, antibody-dependent cell-mediated cytotoxicity or drug conjugates. In this review, we will focus on the interaction between therapeutic antibody and neonatal Fc receptor (FcRn), which is one of the critical factors in determining the circulating antibody half-life. Specifically, we will review the fundamental biology of FcRn, FcRn functions in various organs, Fc mutations designed to modulate binding to FcRn, IgG-based therapeutics that directly exploit FcRn functions and tools and strategies used to study FcRn-IgG interactions. Comprehensive understanding of FcRn-IgG interactions not only allows for development of effective therapeutics, but also avoidance of potential adverse effects.
摘要
如今,大多数有效的新型生物制剂都是 IgG 为基础的分子,这些分子表现出组织靶向特异性,具有良好的临床反应。有几个因素决定了这些产品的疗效,包括靶特异性、血清半衰期和通过补体依赖性细胞毒性、抗体依赖性细胞介导的细胞毒性或药物偶联物发挥的效应功能。在这篇综述中,我们将重点讨论治疗性抗体与新生儿 Fc 受体 (FcRn) 之间的相互作用,这是决定循环抗体半衰期的关键因素之一。具体来说,我们将回顾 FcRn 的基本生物学、FcRn 在各种器官中的功能、设计用于调节与 FcRn 结合的 Fc 突变、直接利用 FcRn 功能的 IgG 治疗药物以及用于研究 FcRn-IgG 相互作用的工具和策略。全面了解 FcRn-IgG 相互作用不仅可以开发有效的治疗药物,还可以避免潜在的不良反应。
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