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人IgDδ重链第一恒定区结构域和铰链区的氨基酸序列。

Amino acid sequence of the first constant region domain and the hinge region of the delta heavy chain of human IgD.

作者信息

Putnam F W, Takahashi N, Tetaert D, Debuire B, Lin L C

出版信息

Proc Natl Acad Sci U S A. 1981 Oct;78(10):6168-72. doi: 10.1073/pnas.78.10.6168.

Abstract

We have determined the amino acid sequence of the first constant (C) region domain (C delta 1) and the hinge region of the delta heavy chain of human IgD WAH and also the sequence of the adjacent COOH-terminal portion of the variable (V) region, including the JH region. Together with the sequence of the Fc fragment already reported, this establishes the complete amino acid sequence of the C region of the human delta chain and confirms the presence of three C region domains in human IgD. Although the CH1 domains of the five classes of human heavy chains have the expected degree of homology (approximately 30%), the homology of the C delta 1 domains of the human and mouse chains is less than that exhibited by the CH1 domains of other pairs of human and mouse heavy chains. The hinge region of the human delta chain has an unusual structure; the NH2-terminal half has four (or five) GalN oligosaccharides attached, whereas the COOH-terminal half lacks carbohydrate, is dissimilar in sequence, and has a high charge. A computer search verified that the GalN-rich segment has a high degree of identity in sequence with the middle portion of the human C mu 2 domain and that the high-charge segment is related to the same sequence. We propose that the two segments of the human delta hinge have a common evolutionary origin and arose by duplication and independent mutation of a hinge exon derived from the ancestral gene for the C mu 2 domain.

摘要

我们已经确定了人IgD WAH δ重链的第一个恒定(C)区结构域(Cδ1)和铰链区的氨基酸序列,以及可变(V)区相邻羧基末端部分(包括JH区)的序列。结合已报道的Fc片段序列,这确定了人δ链C区的完整氨基酸序列,并证实人IgD中存在三个C区结构域。尽管人类五类重链的CH1结构域具有预期程度的同源性(约30%),但人和小鼠链的Cδ1结构域的同源性低于其他成对的人和小鼠重链的CH1结构域所表现出的同源性。人δ链的铰链区具有不寻常的结构;氨基末端一半连接有四个(或五个)GalN寡糖,而羧基末端一半没有碳水化合物,序列不同,且电荷高。计算机搜索证实,富含GalN的片段在序列上与人类Cμ2结构域的中间部分具有高度同一性,且高电荷片段与相同序列相关。我们提出,人δ铰链的这两个片段具有共同的进化起源,是由源自Cμ2结构域祖先基因的铰链外显子的复制和独立突变产生的。

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