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食蟹猴 IgG 亚类的分子和功能特征。

Molecular and functional characterization of cynomolgus monkey IgG subclasses.

机构信息

Department of Protein Science, Amgen, Thousand Oaks, CA 91320, USA.

出版信息

J Immunol. 2011 Jan 1;186(1):341-9. doi: 10.4049/jimmunol.1001685. Epub 2010 Dec 3.

DOI:10.4049/jimmunol.1001685
PMID:21131427
Abstract

Studies for vaccine and human therapeutic Ab development in cynomolgus monkeys (cynos) are influenced by immune responses, with Ab responses playing a significant role in efficacy and immunogenicity. Understanding the nature of cyno humoral immune responses and characterizing the predominant cyno IgG types produced and the Fc-FcγR interactions could provide insight into the immunomodulatory effects of vaccines. Anti-drug Ab responses against human IgG therapeutic candidates in cynos may affect efficacy and safety assessments because of the formation of immune complexes. There is, however, limited information on the structure and function of cyno IgG subclasses and how they compare with human IgG subclasses in Fc-dependent effector functions. To analyze the functional nature of cyno IgG subclasses, we cloned four cyno IgG C regions by using their sequence similarity to other primate IgGs. The four clones, cyno (cy)IGG1, cyIGG2, cyIGG3, cyIGG4, were then used to construct chimeric Abs. The sequence features of cyno IgG subclasses were compared with those of rhesus monkey and human IgG. Our data show that rhesus monkey and cyno IgG C regions are generally highly conserved, with differences in the hinge and hinge-proximal CH2 regions. Fc-dependent effector functions of cyno IgG subclasses were assessed in vitro with a variety of binding and functional assays. Our findings demonstrate distinctive functional properties of cyno IgG subclasses. It is notable that human IgG1 was less potent than cyno IgG1 in cyno FcγR binding and effector functions, with the differences emphasizing the need to carefully interpret preclinical data obtained with human IgG1 therapeutics.

摘要

在食蟹猴(cynos)中进行疫苗和人类治疗性 Ab 开发的研究受到免疫反应的影响,Ab 反应在疗效和免疫原性方面起着重要作用。了解 cyno 体液免疫反应的性质,表征产生的主要 cyno IgG 类型以及 Fc-FcγR 相互作用,可以深入了解疫苗的免疫调节作用。针对 cynos 中人类 IgG 治疗候选药物的抗药物 Ab 反应可能会影响疗效和安全性评估,因为形成了免疫复合物。然而,关于 cyno IgG 亚类的结构和功能以及它们在 Fc 依赖性效应功能方面与人类 IgG 亚类的比较的信息有限。为了分析 cyno IgG 亚类的功能性质,我们使用它们与其他灵长类动物 IgGs 的序列相似性来克隆四个 cyno IgG C 区。然后,使用这四个克隆,即 cyno (cy)IGG1、cyIGG2、cyIGG3 和 cyIGG4,构建嵌合 Ab。比较 cyno IgG 亚类的序列特征与恒河猴和人类 IgG 的序列特征。我们的数据表明,恒河猴和 cyno IgG C 区通常高度保守,铰链和铰链近端 CH2 区存在差异。使用各种结合和功能测定法在体外评估 cyno IgG 亚类的 Fc 依赖性效应功能。我们的发现表明 cyno IgG 亚类具有独特的功能特性。值得注意的是,与 cyno IgG1 相比,人类 IgG1 在 cyno FcγR 结合和效应功能方面的效力较低,这些差异强调需要仔细解释使用人类 IgG1 治疗药物获得的临床前数据。

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