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骆驼单域抗体的一个单环提供的抗原特异性和高亲和力结合。

Antigen specificity and high affinity binding provided by one single loop of a camel single-domain antibody.

作者信息

Desmyter A, Decanniere K, Muyldermans S, Wyns L

机构信息

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

出版信息

J Biol Chem. 2001 Jul 13;276(28):26285-90. doi: 10.1074/jbc.M102107200. Epub 2001 May 7.

Abstract

Detailed knowledge on antibody-antigen recognition is scarce given the unlimited antibody specificities of which only few have been investigated at an atomic level. We report the crystal structures of an antibody fragment derived from a camel heavy chain antibody against carbonic anhydrase, free and in complex with antigen. Surprisingly, this single-domain antibody interacts with nanomolar affinity with the antigen through its third hypervariable loop (19 amino acids long), providing a flat interacting surface of 620 A(2). For the first time, a single-domain antibody is observed with its first hypervariable loop adopting a type-1 canonical structure. The second hypervariable loop, of unique size due to a somatic mutation, reveals a regular beta-turn. The third hypervariable loop covers the remaining hypervariable loops and the side of the domain that normally interacts with the variable domain of the light chain. Specific amino acid substitutions and reoriented side chains reshape this side of the domain and increase its hydrophilicity. Of interest is the substitution of the conserved Trp-103 by Arg because it opens new perspectives to 'humanize' a camel variable domain of heavy chain of heavy chain antibody (VHH) or to 'camelize' a human or a mouse variable domain of heavy chain of conventional antibody (VH).

摘要

鉴于抗体特异性种类无限,而仅有少数在原子水平上得到研究,因此关于抗体 - 抗原识别的详细知识十分匮乏。我们报道了一种源自骆驼重链抗体、针对碳酸酐酶的抗体片段的晶体结构,该结构既有游离状态的,也有与抗原结合的复合物状态的。令人惊讶的是,这种单结构域抗体通过其第三个高变环(19个氨基酸长)以纳摩尔亲和力与抗原相互作用,提供了一个620 Ų的平坦相互作用表面。首次观察到一种单结构域抗体,其第一个高变环采用1型典型结构。由于体细胞突变,第二个高变环大小独特,呈现出规则的β - 转角。第三个高变环覆盖了其余的高变环以及该结构域通常与轻链可变结构域相互作用的一侧。特定的氨基酸取代和重新定向的侧链重塑了该结构域的这一侧,并增加了其亲水性。值得关注的是保守的色氨酸 - 103被精氨酸取代,因为这为“人源化”骆驼重链抗体(VHH)的重链可变结构域或“驼化”传统抗体(VH)的人或小鼠重链可变结构域开辟了新的前景。

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