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首页> 外文期刊>The Journal of Experomental Medicine >Decay-accelerating factor. Genetic polymorphism and linkage to the RCA (regulator of complement activation) gene cluster in humans.
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Decay-accelerating factor. Genetic polymorphism and linkage to the RCA (regulator of complement activation) gene cluster in humans.

机译:衰减加速因子。遗传多态性和人类RCA(补体激活调节剂)基因簇的链接。

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We have investigated the genetic relationships between the human decay-accelerating factor (DAF) and a group of complement components including the C3b/C4b receptor (CR1), C4-binding protein (C4bp), and factor H (H), to which DAF is structurally and functionally related. CR1, C4bp, and H were previously demonstrated to be encoded by a cluster of closely linked genes, which we have designated regulator of complement activation (RCA). Southern blot analysis of genomic DNA using a DAF cDNA probe unraveled the existence of restriction fragment length polymorphism (RFLP) for both Bam HI and Hind III restriction endonucleases. Segregation analysis of these polymorphic fragments in families informative for the segregation of alleles at the CR1, C4BP, and H loci (RCA-haplotypes), demonstrated that, in humans, the gene encoding DAF is located within the RCA gene cluster. No recombinants between DAF and C4BP/CR1 were encountered in 32 informative meioses. In addition, in two individuals showing recombination between the CR1/C4BP and H loci, DAF segregated with the CR1/C4BP segment. Thus, the DAF gene maps closer to the CR1/C4BP loci than to the H gene, from which it can be separated by genetic recombination.
机译:我们已经研究了人类衰变加速因子(DAF)和一组补体成分之间的遗传关系,其中包括C3b / C4b受体(CR1),C4结合蛋白(C4bp)和H因子(H),在结构和功能上相关。先前已证明CR1,C4bp和H由一组紧密相连的基因编码,我们已将其指定为补体激活调节剂(RCA)。使用DAF cDNA探针对基因组DNA进行的Southern印迹分析揭示了Bam HI和Hind III限制性核酸内切酶的限制性片段长度多态性(RFLP)的存在。这些多态性片段在家族中的分离分析对CR1,C4BP和H基因座(RCA-单倍型)等位基因的分离提供了信息,表明在人类中,编码DAF的基因位于RCA基因簇内。 DAF和C4BP / CR1之间没有重组体出现在32个信息丰富的模板中。另外,在显示CR1 / C4BP和H基因座之间重组的两个个体中,DAF与CR1 / C4BP区段分离。因此,DAF基因比H基因更靠近CR1 / C4BP基因座,可以通过基因重组从中分离。

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