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在成年戈谢病中表现出表型不一致的双胞胎对。

Twin pairs showing discordance of phenotype in adult Gaucher's disease.

作者信息

Lachmann R H, Grant I R, Halsall D, Cox T M

机构信息

Department of Medicine, University of Cambridge, Addenbrooke's Hospital, Cambridge, UK.

出版信息

QJM. 2004 Apr;97(4):199-204. doi: 10.1093/qjmed/hch036.

Abstract

BACKGROUND

Non-neuronopathic (type 1) Gaucher's disease, a recessive disorder caused by glucocerebrosidase deficiency, shows marked variability in the severity and extent of clinical expression: many individuals who harbour two mutant alleles remain mildly affected or asymptomatic. Despite much effort, it is not possible accurately to predict disease severity from the genotype, or to identify those patients destined to develop severe disease and meriting early treatment.

AIM

To determine the degree to which variance in Gaucher disease is determined by non-heritable factors.

DESIGN

Case reports of monozygotic and dizygotic twin pairs.

RESULTS

For the monozygotic twin pair, homozygous for the frequent N370S glucocerebrosidase allele, there was no evidence that significant lipid storage was ever initiated in the unaffected twin. In contrast, pathological storage of glucocerebroside has been present in the macrophages of both members of the dizygotic twin pair (compound heterozygotes for the N370S and L444P alleles) from an early age but, by the age of 57 years, only one has developed symptoms.

DISCUSSION

Non-heritable factors influence Gaucher disease expression in genetically predisposed individuals. Understanding the interactions between heritable and non-heritable factors will be critical for an analysis of pathogenesis, and the treatment of individuals predisposed to Gaucher disease.

摘要

背景

非神经元型(1型)戈谢病是一种由葡糖脑苷脂酶缺乏引起的隐性疾病,其临床表现在严重程度和范围上存在显著差异:许多携带两个突变等位基因的个体症状较轻或无症状。尽管付出了很多努力,但仍无法根据基因型准确预测疾病严重程度,也无法识别那些注定会发展为严重疾病并值得早期治疗的患者。

目的

确定非遗传因素在多大程度上决定戈谢病的差异。

设计

单卵双胞胎和双卵双胞胎的病例报告。

结果

对于同是常见的N370S葡糖脑苷脂酶等位基因纯合子的单卵双胞胎,没有证据表明未受影响的双胞胎曾开始显著的脂质蓄积。相比之下,双卵双胞胎(N370S和L444P等位基因的复合杂合子)的两名成员从幼年起巨噬细胞中就存在葡糖脑苷脂的病理性蓄积,但到57岁时,只有一人出现了症状。

讨论

非遗传因素会影响具有遗传易感性个体的戈谢病表现。了解遗传因素与非遗传因素之间的相互作用对于分析发病机制以及治疗戈谢病易感个体至关重要。

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