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源自天然骆驼重链抗体的独特单域抗原结合片段。

Unique single-domain antigen binding fragments derived from naturally occurring camel heavy-chain antibodies.

作者信息

Muyldermans S, Lauwereys M

机构信息

Ultrastructure, Vlaams Interuniversitair Instituut voor Biotechnologie, Vrije Universiteit Brussel, Paardenstraat 65, B-1640 Sint Genesius Rode, Belgium.

出版信息

J Mol Recognit. 1999 Mar-Apr;12(2):131-40. doi: 10.1002/(SICI)1099-1352(199903/04)12:2<131::AID-JMR454>3.0.CO;2-M.

DOI:10.1002/(SICI)1099-1352(199903/04)12:2<131::AID-JMR454>3.0.CO;2-M
PMID:10398404
Abstract

The humoral immune response of camels, dromedaries and llamas includes functional antibodies formed by two heavy chains and no light chains. The amino acid sequence of the variable domain of the naturally occurring heavy-chain antibodies reveals the necessary adaptations to compensate for the absence of the light chain. In contrast to the conventional antibodies, a large proportion of the heavy-chain antibodies acts as competitive enzyme inhibitors. Studies on the dromedary immunoglobulin genes start to shed light on the ontogeny of these heavy-chain antibodies. The presence of the heavy-chain antibodies and the possibility of immunizing a dromedary allows for the production of antigen binders consisting of a single domain only. These minimal antigen-binding fragments are well expressed in bacteria, bind the antigen with affinity in the nM range and are very stable. We expect that such camelid single domain antibodies will find their way into a number of biotechnological or medical applications. The structure of the camelid single domain is homologous to the human VH, however, the antigen-binding loop structures deviate fundamentally from the canonical structures described for human or mouse VHs. This has two additional advantages: (1) the camel or llama derived single domain antibodies might be an ideal scaffold for anti-idiotypic vaccinations; and (2) the development of smaller peptides or peptide mimetic drugs derived from of the antigen binding loops might be facilitated due to their less complex antigen binding site.

摘要

骆驼、单峰驼和美洲驼的体液免疫反应包括由两条重链而非轻链形成的功能性抗体。天然重链抗体可变区的氨基酸序列显示出为弥补轻链缺失而进行的必要适应性变化。与传统抗体不同,很大一部分重链抗体可作为竞争性酶抑制剂。对单峰驼免疫球蛋白基因的研究开始揭示这些重链抗体的个体发生情况。重链抗体的存在以及对单峰驼进行免疫的可能性使得仅由单个结构域组成的抗原结合物得以产生。这些最小的抗原结合片段在细菌中表达良好,以纳摩尔范围的亲和力结合抗原,并且非常稳定。我们预计此类骆驼科动物单结构域抗体将在许多生物技术或医学应用中得到应用。骆驼科动物单结构域的结构与人类VH结构同源,然而,其抗原结合环结构与人类或小鼠VH所描述的典型结构有根本差异。这还有另外两个优点:(1)骆驼或美洲驼来源的单结构域抗体可能是抗独特型疫苗接种的理想支架;(2)由于其抗原结合位点不太复杂,可能会促进从抗原结合环衍生出更小的肽或肽模拟药物的开发。

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