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四种新型ε链mRNA的特征分析及啮齿动物和人类免疫球蛋白E基因的比较分析。

Characterization of four novel epsilon chain mRNA and a comparative analysis of genes for immunoglobulin E in rodents and man.

作者信息

Hellman L

机构信息

Department of Immunology, University of Uppsala, Sweden.

出版信息

Eur J Immunol. 1993 Jan;23(1):159-67. doi: 10.1002/eji.1830230126.

Abstract

The nucleotide sequence of the 3' region of the epsilon chain gene for human IgE is presented. A comparison of the entire region from 5' of exon C1 to the M2 exon of the mouse, rat and human epsilon chain genes shows that the overall structure of the epsilon chain gene have changed only minimally during the 60-70 million years of evolutionary separation between rodents and man. We have previously shown that a number of rearrangements larger than 10 bp have relatively recently occurred in the C4/M1 intron of the rat or the mouse epsilon chain genes. A majority of these rearrangements were found within or in close proximity to repetitive sequences of Z-DNA-forming potential (CA dinucleotide repeats). The C4/M1 intron has evolved very rapidly, to such an extent that no apparent homology can be detected between rodents and man. Only remnants of the repetitive sequences are present in man, supporting the theory that repetitive sequences having Z-DNA-forming properties may play a role in the evolution of the eucaryote genome by promoting recombinations, leading to a rapid evolutionary drift of sequences in close proximity to these repeats. We report here the characterization of the membrane domains of human IgE and four novel mRNA transcribed from the human epsilon chain locus. The primary structures have been determined by polymerase chain reaction cloning and nucleotide sequence analysis. All five mRNA contain the C3 domain and the membrane exon 2 (M2). Due to frame shifts caused by novel splice sites or novel splice-site combinations, the proteins encoded by three out of these four novel mRNA differ in their carboxy-terminal end from the classical secreted or membrane-bound immunoglobulins. Northern blot analysis shows significant levels of at least three out of these four novel mRNA in an IgE-producing human cell line. One of the mRNA encodes a transmembrane-like structure which has characters in common with the transmembrane region of the CD3 components of the T cell receptor complex (CD3 gamma, delta and epsilon). This indicates that IgE-producing B cells possibly have two separate signal-transducing systems. A comparison of the classical membrane anchoring domain of the human & chain with a panel of immunoglobulin membrane domains from fish to higher mammals is presented. A tyrosine and a glutamine residue is found to be conserved between all cytoplasmic domains of all post-switch immunoglobulin classes indicating a functional conservation of these amino acid residues.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

本文展示了人类IgE ε链基因3'区域的核苷酸序列。对小鼠、大鼠和人类ε链基因从外显子C1的5'端到M2外显子的整个区域进行比较,结果表明,在啮齿动物和人类6000万至7000万年的进化分离过程中,ε链基因的整体结构变化极小。我们之前已经表明,大鼠或小鼠ε链基因的C4/M1内含子中最近发生了一些大于10 bp的重排。这些重排中的大多数位于具有形成Z-DNA潜力的重复序列(CA二核苷酸重复序列)内部或附近。C4/M1内含子进化非常迅速,以至于在啮齿动物和人类之间无法检测到明显的同源性。人类中仅存在重复序列的残余部分,这支持了具有形成Z-DNA特性的重复序列可能通过促进重组在真核生物基因组进化中发挥作用的理论,导致与这些重复序列紧邻的序列快速进化漂移。我们在此报告人类IgE膜结构域以及从人类ε链基因座转录的四种新mRNA的特征。其一级结构已通过聚合酶链反应克隆和核苷酸序列分析确定。所有五种mRNA都包含C3结构域和膜外显子2(M2)。由于新的剪接位点或新的剪接位点组合导致的移码,这四种新mRNA中的三种所编码的蛋白质在其羧基末端与经典的分泌型或膜结合型免疫球蛋白不同。Northern印迹分析表明,在产生IgE的人类细胞系中,这四种新mRNA中的至少三种具有显著水平。其中一种mRNA编码一种类似跨膜的结构,它与T细胞受体复合物的CD3成分(CD3γ、δ和ε)的跨膜区域具有共同特征。这表明产生IgE的B细胞可能有两个独立的信号转导系统。本文展示了人类ε链的经典膜锚定结构域与从鱼类到高等哺乳动物的一组免疫球蛋白膜结构域的比较。发现在所有转换后免疫球蛋白类别的所有细胞质结构域之间,酪氨酸和谷氨酰胺残基是保守的,这表明这些氨基酸残基具有功能保守性。(摘要截断于400字)

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