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人类免疫球蛋白同种型:对免疫原性的可能影响。

Human immunoglobulin allotypes: possible implications for immunogenicity.

机构信息

School of Immunity and Infection, College of Medical and Dental Sciences, University of Birmingham, Birmingham B15 2TT, UK.

出版信息

MAbs. 2009 Jul-Aug;1(4):332-8. doi: 10.4161/mabs.1.4.9122.

Abstract

More than twenty recombinant monoclonal antibodies are approved as therapeutics. Almost all of these are based on the whole IgG isotype format, but vary in the origin of the variable regions between mouse (chimeric), humanized mouse and fully human sequences; all of those with whole IgG format employ human constant region sequences. Currently, the opposing merits of the four IgG subclasses are considered with respect to the in vivo biological activities considered to be appropriate to the disease indication being treated. Human heavy chain genes also exhibit extensive structural polymorphism(s) and, being closely linked, are inherited as a haplotype. Polymorphisms (allotypes) within the IgG isotype were originally discovered and described using serological reagents derived from humans; demonstrating that allotypic variants can be immunogenic and provoke antibody responses as a result of allo-immunization. The serologically defined allotypes differ widely within and between population groups; therefore, a mAb of a given allotype will, inevitably, be delivered to a cohort of patients homozygous for the alternative allotype. This publication reviews the serologically defined human IgG allotypes and considers the potential for allotype differences to contribute to or potentiate immunogenicity.

摘要

已有二十多种重组单克隆抗体被批准作为治疗药物。这些药物几乎全部基于完整 IgG 同种型,但在可变区的来源上存在差异,包括鼠(嵌合)、人源化鼠和全人序列;所有这些具有完整 IgG 同种型的抗体都采用人恒定区序列。目前,根据治疗疾病的适应证,考虑了四种 IgG 亚类的相反优势。人类重链基因也表现出广泛的结构多态性(同种异型),并且由于紧密连锁,作为单倍型遗传。最初使用源自人类的血清学试剂发现并描述了 IgG 同种型内的多态性(同种异型);证明同种异型变体可以作为同种异体免疫原而引发抗体反应。在人群中,血清学定义的同种异型在内部和群体之间差异很大;因此,给定同种异型的 mAb 将不可避免地被传递给另一种同种异型纯合的患者群体。本出版物综述了血清学定义的人类 IgG 同种异型,并考虑了同种异型差异是否会导致或增强免疫原性的可能性。

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