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Mutations at the lysosomal acid cholesteryl ester hydrolase gene locus in Wolman disease.

机译:沃尔曼病中的溶酶体酸胆固醇酯水解酶基因位点的突变。

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摘要

The genomic sequences encoding the human lysosomal acid lipase/cholesteryl esterase (sterol esterase; EC 3.1.1.13) have been isolated and sequenced, and the information has been used to identify mutations in both alleles of the gene from a patient with Wolman disease, an autosomal recessive lysosomal lipid storage disorder. The genomic locus consists of 10 exons spread over 36 kb. The 5' flanking region is G+C-rich and has characteristics of a "housekeeping" gene promoter. One of the identified mutations involves the insertion of a T residue after position 634, resulting in the appearance of an in-frame translation stop signal 13 codons downstream. The second mutation is a T-to-C transition at nucleotide 638. This results in a leucine-to-proline substitution at amino acid 179 and is predicted to lead to the disruption of the alpha-helical structure in a highly conserved region of the protein. These mutations are each capable of completely disrupting the catalytic function of the lysosomal acid cholesteryl ester hydrolase; their presence can account for the extreme phenotype of the lysosomal lipid storage disorder manifested in members of this patient's family.
机译:已经分离并测序了编码人溶酶体酸性脂肪酶/胆固醇酯酶(甾醇酯酶; EC 3.1.1.13)的基因组序列,并将该信息用于鉴定患有沃尔曼氏病(Wolman病)的患者的两个基因等位基因的突变。常染色体隐性遗传型溶酶体脂质贮积病。基因组基因座由分布在36 kb的10个外显子组成。 5'侧翼区富含G + C,并具有“管家”基因启动子的特征。所鉴定的突变之一涉及在位置634之后插入T残基,导致在下游出现框内翻译终止信号13密码子。第二个突变是核苷酸638处的T到C过渡。这会导致氨基酸179上的亮氨酸到脯氨酸取代,并被认为会导致其高度保守区域的α螺旋结构破坏。蛋白。这些突变均能够完全破坏溶酶体酸胆固醇酯水解酶的催化功能。它们的存在可以解释该患者家庭成员中出现的溶酶体脂质贮积病的极端表型。

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