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一种由杂交瘤抗体识别的人类类风湿因子上的常见独特型。

A common idiotope on human rheumatoid factors identified by a hybridoma antibody.

作者信息

Carson D A, Fong S

出版信息

Mol Immunol. 1983 Oct;20(10):1081-7. doi: 10.1016/0161-5890(83)90116-5.

Abstract

Human monoclonal and polyclonal anti-IgG autoantibodies [rheumatoid factors (RFs)] are composed primarily of kappa light chains, and may display cross-reactive idiotypes. However, the nature of the shared idiotope(s) has remained unclear. We have prepared a murine hybridoma antibody (17-109) that recognizes an idiotope present on 30% (3/10) of human IgM-RF paraproteins, and absent on immunoglobulins without RF activity. The idiotope was measurable on isolated, intact kappa light chains, but not on light-chain tryptic peptides, nor on isolated heavy chains. A comparison of the binding to 17-109 of five IgM-RF paraproteins, with known kappa chain amino acid sequences, suggested a relationship between the idiotope recognized by the hybridoma and the complementarity-determining regions. The serum of patients with rheumatoid arthritis contained idiotope positive material that bound specifically to a 17-109 immunoadsorbent column. Moreover, the 17-109 anti-idiotope antibody partially inhibited the binding to IgG of IgM-RF and IgA-RF in serum, but did not effect the binding to antigen of IgM and IgA anti-tetanus toxoid antibodies. These results suggest that a significant proportion of IgM-RF paraproteins share an idiotope located at or near the complementarity-determining regions of the kappa light chain. Human serum RFs include a kappa light chain family that is idiotopically related to the kappa chains on IgM-RF paraproteins.

摘要

人单克隆和多克隆抗IgG自身抗体[类风湿因子(RFs)]主要由κ轻链组成,并且可能表现出交叉反应性独特型。然而,共享独特型的性质仍不清楚。我们制备了一种鼠杂交瘤抗体(17 - 109),它识别存在于30%(3/10)的人IgM - RF副蛋白上的独特型,而在没有RF活性的免疫球蛋白上不存在。该独特型在分离的完整κ轻链上可检测到,但在轻链胰蛋白酶肽段上以及分离的重链上均检测不到。对五个已知κ链氨基酸序列的IgM - RF副蛋白与17 - 109的结合进行比较,提示杂交瘤识别的独特型与互补决定区之间存在关联。类风湿性关节炎患者的血清中含有与17 - 109免疫吸附柱特异性结合的独特型阳性物质。此外,17 - 109抗独特型抗体部分抑制血清中IgM - RF和IgA - RF与IgG的结合,但不影响IgM和IgA抗破伤风类毒素抗体与抗原的结合。这些结果表明,相当一部分IgM - RF副蛋白共享位于κ轻链互补决定区或其附近的独特型。人血清RFs包括一个独特型与IgM - RF副蛋白上的κ链相关的κ轻链家族。

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