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对Ia.7抗体具有明显公共独特型特异性的异种抗体部分针对Vκ21D和E亚组标记。

Xenogeneic antibodies with apparent public idiotypic specificity for anti-Ia.7 antibodies are directed in part against V kappa 21D and E subgroup marker.

作者信息

Devaux C A, Pierres M, Epstein S L, Sachs D H

出版信息

J Immunol. 1986 May 15;136(10):3760-6.

PMID:3084643
Abstract

Public idiotypes (IdX) expressed on monoclonal antibodies (mAb) against a monomorphic alpha-chain determinant of the I-E molecule (Ia.7 epitope cluster I) have been studied by using xenogeneic anti-Id reagents derived from pig, rabbit, and rat. IdX+ anti-Ia.7 mAb were recently demonstrated to be structurally related by a high frequency expression of the V kappa 21E light chain subgroup. This raised the question of whether V region determinants of the IdX were related to V kappa 21E sequences or whether they were unique to hypervariable regions of Ia.7 binding antibodies. To clarify this question, the possible association between the expression of the public Id (IdX(s)Ia.7) and the presence of V kappa sequences (V kappa 21E and/or J kappa segment) was examined. The reactivity of the anti-Id reagents with a random panel of 28 myeloma products (each containing a light chain from one of the different V kappa 21 subgroups) was studied by assaying the ability of these mAb to inhibit the binding between the anti-Id and anti-Ia.7 mAb. This analysis demonstrates that what has previously been defined as IdX Ia.7 includes determinants shared by V kappa 21E and V kappa 21D light chain V regions. The structures recognized are expressed irrespective of the J kappa segment. In addition, this study demonstrates interspecies variation in immune responses to such V kappa 21E antigenic determinants. Additional IdX components are found on anti-Ia.7 mAb but not on other V kappa 21E or D proteins. Thus V region subgroup considerations have crucial implications for Id characterization. In addition, this work describes the first division of the V kappa 21 subgroup into component parts by a mAb.

摘要

利用源自猪、兔和大鼠的异种抗独特型试剂,对针对I-E分子单态性α链决定簇(Ia.7表位簇I)的单克隆抗体(mAb)上表达的公共独特型(IdX)进行了研究。最近发现,IdX+抗Ia.7 mAb在结构上与Vκ21E轻链亚群的高频表达相关。这就提出了一个问题,即IdX的V区决定簇是与Vκ21E序列相关,还是Ia.7结合抗体高变区所特有的。为了阐明这个问题,研究了公共Id(IdX(s)Ia.7)的表达与Vκ序列(Vκ21E和/或Jκ片段)的存在之间的可能关联。通过检测这些mAb抑制抗独特型与抗Ia.7 mAb之间结合的能力,研究了抗独特型试剂与一组28种骨髓瘤产物(每种含有来自不同Vκ21亚群之一的轻链)的反应性。该分析表明,先前定义为IdX Ia.7的包括Vκ21E和Vκ21D轻链V区共有的决定簇。所识别的结构不依赖于Jκ片段而表达。此外,本研究表明,对这种Vκ21E抗原决定簇的免疫反应存在种间差异。在抗Ia.7 mAb上发现了其他IdX成分,但在其他Vκ21E或D蛋白上未发现。因此,V区亚群的考虑对独特型的表征具有至关重要的意义。此外,这项工作描述了通过一种mAb首次将Vκ21亚群划分为不同组成部分。

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