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菊粉结合型骨髓瘤蛋白重链间的序列变异

Sequence variation among heavy chains from inulin-binding myeloma proteins.

作者信息

Vrana M, Rudikoff S, Potter M

出版信息

Proc Natl Acad Sci U S A. 1978 Apr;75(4):1957-61. doi: 10.1073/pnas.75.4.1957.

Abstract

The entire sequences of the variable region of four heavy chains from BALB/c inulin-binding myeloma proteins have been determined. Among the four proteins there are six amino acid differences, all of which occur in the framework portion of the variable region. All of the six amino acid substitutions can be explained by single base mutations at the DNA level. The pattern of diversity in these proteins is compared to a previously reported group of heavy chains from phosphorylcholine-binding myeloma proteins. Unlike the phosphorylcholine-binding proteins, which (with the exception of two that are identical) have size and sequence differences in their complementarity regions, the inulin-binding heavy chains all have identical complementarity regions with H3 being extremely short. The pattern of variation observed in the anti-inulin heavy chains appears to be most easily explained by a somatic mutation mechanism. However, because none of the substitutions occur in complementarity-determining regions, they presumably would have no selective advantage and would not alter binding specificity. These proteins have further been shown to have crossreacting antigenic determinants (idiotypes). Five of the six sequence differences observed occur at positions that are internal in the molecule and thus presumably would not account for the idiotypic differences. These results suggest that most of the observed idiotypic crossreactivities will be due to differences in the light chains of the anti-inulin proteins.

摘要

已确定来自BALB/c菊粉结合骨髓瘤蛋白的四条重链可变区的完整序列。在这四种蛋白中存在六个氨基酸差异,所有这些差异都出现在可变区的框架部分。这六个氨基酸替换都可以通过DNA水平的单碱基突变来解释。将这些蛋白中的多样性模式与先前报道的一组磷酸胆碱结合骨髓瘤蛋白的重链进行了比较。与磷酸胆碱结合蛋白不同(除了两个相同的蛋白外),它们在互补区存在大小和序列差异,菊粉结合重链的互补区都相同,其中H3非常短。在抗菊粉重链中观察到的变异模式似乎最容易用体细胞突变机制来解释。然而,由于没有一个替换发生在互补决定区,它们大概没有选择优势,也不会改变结合特异性。这些蛋白进一步被证明具有交叉反应性抗原决定簇(独特型)。观察到的六个序列差异中有五个发生在分子内部的位置,因此大概不会导致独特型差异。这些结果表明,观察到的大多数独特型交叉反应性将归因于抗菊粉蛋白轻链的差异。

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