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Evidence for linkage between the loci coding for the binding protein for the fourth component of human complement (C4BP) and for the C3b/C4b receptor.

机译:编码人类补体第四组分(C4BP)结合蛋白和C3b / C4b受体结合蛋白的基因座之间连锁的证据。

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摘要

Three pedigrees informative for the segregation of genetic variants of the binding protein for the fourth component of complement (C4BP) and C3b/C4b receptor (C3bR) have been identified. There were 10 informative meioses with no recombinants, indicating a close linkage between the loci encoding C4BP and C3bR, C4BP and C3bR [maximum lod (logarithm of odds of linkage) score: 2.4 at recombinant fraction = 0.0]. In addition, in the four unrelated individuals who were doubly heterozygous (C4BP*1, C4BP*2, C3bR*A, C3bR*B), the infrequent allele C4BP*2 segregated together with the uncommon allele C3bR*B, supporting the hypothesis of linkage between C4BP and C3bR and suggesting that linkage disequilibrium exists between these particular alleles. We conclude that the loci encoding C3bR and C4BP, two functionally related molecules, are linked.
机译:已鉴定出三个谱系,可为补体第四组分(C4BP)和C3b / C4b受体(C3bR)的结合蛋白的遗传变异提供信息。有10个信息丰富的片段,没有重组体,表明编码C4BP和C3bR,C4BP和C3bR的基因座之间有紧密的联系[最大lod(联系几率的对数)得分:2.4,重组分数= 0.0]。此外,在四个杂合子无关的四个无关个体(C4BP * 1,C4BP * 2,C3bR * A,C3bR * B)中,罕见的等位基因C4BP * 2与罕见的等位基因C3bR * B分离,支持了以下假设C4BP和C3bR之间存在连锁关系,这表明这些特定等位基因之间存在连锁不平衡。我们得出结论,编码C3bR和C4BP,两个功能相关的分子的基因座是链接的。

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