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C7 M/N protein polymorphism typing applied to inherited deficiencies of human complement proteins C6 and C7.

机译:C7 M / N蛋白多态性分型适用于人类补体蛋白C6和C7的遗传缺陷。

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摘要

C7 M/N typing, the determination of the complement component C7 M/N phenotypes, was successfully used in family studies to trace haplotypes bearing C7 deficiency genes. Furthermore, it was shown to be preferable to C7 allotyping based on isoelectric focusing (IEF) since it distinguishes two common alleles (C7*M and C7*N), whereas one common C7 IEF allele (C7*1) predominates in most populations. It is also the more sensitive method, as it enabled detection of very low amounts of abnormal C7 molecules in the third generation of a combined subtotal C6/C7-deficient subject and thus confirmed that this partial deficiency gene is not silent in heterozygotes. In this respect C7 M/N typing is even more informative than DNA restriction fragment length polymorphism typing which will assess the presence but not necessarily the functional status of a gene. C6 and C7 genes are tightly linked and therefore C7 M/N typing was also applied to tracing C6 deficiency genes in families. C6/C7 haplotype analysis of South African C6-deficient (C6Q0) subjects revealed a strong allelic association of C6*Q0 and C7*M.
机译:C7 M / N分型是补体成分C7 M / N表型的确定,已成功用于家庭研究中,以追踪带有C7缺陷基因的单倍型。此外,由于它可以区分两个常见的等位基因(C7 * M和C7 * N),因此显示出优于基于等电聚焦(IEF)的C7异型分型,而在大多数人群中,一个常见的C7 IEF等位基因(C7 * 1)占优势。这也是一种更灵敏的方法,因为它可以在第三代C6 / C7缺陷综合人群中检测到极少量的异常C7分子,因此证实了该部分缺陷基因在杂合子中不是沉默的。在这方面,C7 M / N分型比DNA限制性片段长度多态性分型更具信息性,DNA限制性片段长度多态性分型将评估基因的存在,但不一定评估基因的功能状态。 C6和C7基因紧密相连,因此C7 M / N分型也适用于追踪家庭中的C6缺陷基因。南非C6缺陷(C6Q0)受试者的C6 / C7单倍型分析显示,C6 * Q0和C7 * M有很强的等位基因关联。

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