Das S, Levinson B, Vulpe C, Whitney S, Gitschier J, Packman S
Department of Pediatrics, University of California, San Francisco 94143-0724.
Am J Hum Genet. 1995 Mar;56(3):570-6.
The connective-tissue disorder occipital horn syndrome (OHS) is hypothesized to be allelic to Menkes disease. The two diseases have different clinical presentations but have a similar abnormality of copper transport. Mice hemizygous for the blotchy allele of the X-linked mottled locus have similar connective-tissue defects as OHS and may represent a mouse model of this disease. We have analyzed the Menkes/mottled copper-transporting ATPase in these two potentially homologous disorders and have identified similar splicing mutations in both. Some expression of normal mRNA was detectable by reverse transcription-PCR in the mutant tissues. These findings contrast with the more debilitating mutations observed in Menkes disease and suggest that low amounts of an otherwise normal protein product could result in the relatively mild phenotype of OHS and of the blotchy mouse.
结缔组织疾病枕角综合征(OHS)被推测与门克斯病等位基因相同。这两种疾病有不同的临床表现,但铜转运存在相似异常。X连锁斑驳位点的斑驳等位基因半合子小鼠具有与OHS相似的结缔组织缺陷,可能代表了这种疾病的小鼠模型。我们分析了这两种潜在同源疾病中的门克斯/斑驳铜转运ATP酶,并在两者中都发现了相似的剪接突变。通过逆转录聚合酶链反应在突变组织中可检测到正常mRNA的一些表达。这些发现与在门克斯病中观察到的更严重的突变形成对比,表明正常蛋白质产物的少量存在可能导致OHS和斑驳小鼠相对较轻的表型。
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