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天然小鼠和人类抗体与源自种系VH链的肽结合。进化保守的自身结合位点的证据。

Natural mouse and human antibodies bind to a peptide derived from a germline VH chain. Evidence for evolutionary conserved self-binding locus.

作者信息

Kaveri S V, Kang C Y, Köhler H

机构信息

IDEC Pharmaceuticals Corporation, La Jolla, CA 92037.

出版信息

J Immunol. 1990 Dec 15;145(12):4207-13.

PMID:2124238
Abstract

Murine antibodies derived from the V1 S107/T15 germline structure combined with Vk 22 L chains express the property of self-binding. Previous studies have shown that the self-binding is mediated by the Fab fragment involving structures of the hapten binding site. The molecular locus of self-binding has also been identified by showing that a peptide derived from the CDR2/FR3 region of the V1 S107 H chain inhibits self-binding. We have addressed the question of whether self-binding antibodies interact with peptides that inhibit self-binding. We found that labeled TEPC15 (T15) binds to immobilized VH (50-73) peptide; the peptide binding is specific because different CDR peptides and other unrelated peptides do not inhibit this binding. Furthermore, the hapten phosphorylcholine is a potent inhibitor for the T15-peptide binding. We have demonstrated the presence of naturally occurring antibodies that bind to the T15H(50-73) peptide in the sera of different strains of mice and also in humans, indicating that the CDR2/FR3 sequence of T15 is a conserved Id determining region. We have isolated peptide-specific antibodies from pooled normal human Ig preparations. Human anti-peptide antibodies have self-binding properties similar to their murine counterparts. This interspecies conserved peptide binding of antibodies that are self-binding indicates the existence of an evolutionarily important and biologically active site.

摘要

源自V1 S107/T15胚系结构并与Vk 22轻链结合的鼠源抗体具有自身结合特性。先前的研究表明,这种自身结合是由涉及半抗原结合位点结构的Fab片段介导的。通过显示源自V1 S107重链CDR2/FR3区域的肽可抑制自身结合,自身结合的分子位点也已得到确定。我们探讨了自身结合抗体是否与抑制自身结合的肽相互作用这一问题。我们发现标记的TEPC15(T15)与固定化的VH(50 - 73)肽结合;这种肽结合具有特异性,因为不同的CDR肽和其他无关肽不会抑制这种结合。此外,半抗原磷酸胆碱是T15 - 肽结合的有效抑制剂。我们已经证明在不同品系小鼠的血清以及人类血清中存在与T15H(50 - 73)肽结合的天然抗体,这表明T15的CDR2/FR3序列是一个保守的独特型决定区域。我们从混合的正常人Ig制剂中分离出了肽特异性抗体。人抗肽抗体具有与其鼠源对应物相似的自身结合特性。这种自身结合抗体的种间保守肽结合表明存在一个具有进化重要性和生物活性的位点。

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