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两名患有严重2型邓尼根型家族性部分脂肪营养不良的姐妹中存在LMNA剪接突变。

A LMNA splicing mutation in two sisters with severe Dunnigan-type familial partial lipodystrophy type 2.

作者信息

Morel Chantal F, Thomas Mary Ann, Cao Henian, O'Neil Caroline H, Pickering J Geoffrey, Foulkes William D, Hegele Robert A

机构信息

Blackburn Cardiovascular Genetics Laboratory, Robarts Research Institute, London, Ontario, Canada.

出版信息

J Clin Endocrinol Metab. 2006 Jul;91(7):2689-95. doi: 10.1210/jc.2005-2746. Epub 2006 Apr 24.

DOI:10.1210/jc.2005-2746
PMID:16636128
Abstract

CONTEXT

To date, all cases of familial partial lipodystrophy type 2 (FPLD2; Mendelian Inheritance in Man 151660) result from missense mutations in LMNA, which encodes nuclear lamin A/C (Mendelian Inheritance in Man 150330).

OBJECTIVE

The objective of the study was to carry out mutational analysis of LMNA in two sisters with a particularly severe FPLD2 phenotype.

DESIGN

This was a descriptive case report with molecular studies.

SETTING

The study was conducted at a referral center.

PATIENTS

We report two sisters of South Asian origin. The first presented with acanthosis nigricans at age 5 yr, diabetes with insulin resistance, hypertension and hypertriglyceridemia at age 13 yr, and partial lipodystrophy starting at puberty. Her sister and their mother had a similar metabolic profile and physical features, and their mother died of vascular disease at age 32 yr.

INTERVENTIONS

There were no interventions.

MAIN OUTCOME MEASURES AND RESULTS

LMNA sequencing showed that the sisters were each heterozygous for a novel G>C mutation at the intron 8 consensus splice donor site, which was absent from the genomes of 300 healthy individuals. The retention of intron 8 in mRNA predicted a prematurely truncated lamin A isoform (516 instead of 664 amino acids) with 20 nonsense 3'-terminal residues. The mutant lamin A isoform failed to interact normally with emerin and failed to localize to the nuclear envelope.

CONCLUSIONS

This is the first LMNA splicing mutation to be associated with FPLD2, and it causes a severe clinical and metabolic phenotype.

摘要

背景

迄今为止,所有2型家族性部分脂肪营养不良(FPLD2;《人类孟德尔遗传》编号151660)病例均由LMNA基因的错义突变导致,该基因编码核纤层蛋白A/C(《人类孟德尔遗传》编号150330)。

目的

本研究旨在对两名具有特别严重FPLD2表型的姐妹进行LMNA基因突变分析。

设计

这是一项带有分子研究的描述性病例报告。

地点

研究在一家转诊中心进行。

患者

我们报告了两名南亚裔姐妹。第一名患者5岁时出现黑棘皮病,13岁时出现伴有胰岛素抵抗的糖尿病、高血压和高甘油三酯血症,青春期开始出现部分脂肪营养不良。她的妹妹和母亲有相似的代谢特征和身体特征,她们的母亲32岁时死于血管疾病。

干预措施

未采取干预措施。

主要观察指标及结果

LMNA基因测序显示,这两名姐妹在第8内含子共有剪接供体位点均为一种新的G>C突变的杂合子,300名健康个体的基因组中未发现该突变。mRNA中第8内含子的保留预测会产生一种截短的核纤层蛋白A异构体(516个氨基酸而非664个氨基酸),其3'端有20个无义残基。突变的核纤层蛋白A异构体无法与emerin正常相互作用,也无法定位于核膜。

结论

这是首个与FPLD2相关的LMNA剪接突变,它导致了严重的临床和代谢表型。

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