首页> 美国卫生研究院文献>Journal of Medical Genetics >Evidence for exclusion of a mutation in NRAMP as the cause of familial disseminated atypical mycobacterial infection in a Maltese kindred.
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Evidence for exclusion of a mutation in NRAMP as the cause of familial disseminated atypical mycobacterial infection in a Maltese kindred.

机译:有证据表明马耳他血统的家族性非典型分枝杆菌感染是由NRAMP突变引起的。

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摘要

In mice, susceptibility to intracellular infections in inbred strains is controlled by a single locus, Lsh/Ity/Bcg, and the gene responsible has been cloned and designated Nramp (Natural resistance associated macrophage protein). We have identified a group of related children who appear to have a single gene defect, inherited recessively, which results in increased susceptibility to myocabacterial infection. The immunological defect observed in the affected children resembles that in mice homozygous for the Lsh/Ity/Bcg susceptible allele. To test the hypothesis that a mutation in NRAMP is responsible for the immunodeficiency observed in the affected children, we have typed eight markers in the region of human 2q34-q37 where NRAMP, the human homologue of Nramp, maps. We have shown discordance with the defect in one family and the chromosomes in the three affected children have different haplotypes making it unlikely that inheritance of an ancestral mutation in the NRAMP gene is the cause of increased mycobacterial susceptibility in this group of children.
机译:在小鼠中,近交菌株对细胞内感染的易感性受单个基因座Lsh / Ity / Bcg的控制,并且负责的基因已被克隆并命名为Nramp(与自然抗性相关的巨噬细胞蛋白)。我们已经鉴定出一组相关儿童,这些儿童似乎具有隐性遗传的单个基因缺陷,从而导致对分支杆菌感染的敏感性增加。在受影响的儿童中观察到的免疫缺陷类似于在Lsh / Ity / Bcg易感等位基因纯合的小鼠中。为了检验NRAMP突变导致患病儿童免疫缺陷的假说,我们在人2q34-q37区域输入了8个标记,其中NRAMP是Nramp的人类同源物。我们已经显示出与一个家庭的缺陷不一致,并且三个受影响的儿童中的染色体具有不同的单倍型,这使得NRAMP基因的祖先突变的遗传不可能成为该组儿童中分枝杆菌敏感性增加的原因。

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