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遗传性淋巴水肿的发病年龄。

Age of onset in hereditary lymphedema.

作者信息

Levinson Kara L, Feingold Eleanor, Ferrell Robert E, Glover Thomas W, Traboulsi Elias I, Finegold David N

机构信息

Department of Human Genetics, University of Pittsburgh, Pittsburgh, Pennsylvania 15261, USA.

出版信息

J Pediatr. 2003 Jun;142(6):704-8. doi: 10.1067/mpd.2003.235.

Abstract

OBJECTIVE

To characterize age of onset patterns and penetrance in hereditary lymphedema, including differences caused by sex and genetic heterogeneity.

STUDY DESIGN

Kaplan-Meier analysis of three family cohorts with autosomal dominant lymphedema: (1) five families with unique mutations in FLT4, (2) 16 families with unique mutations in FOXC2, and (3) 77 families with no mutations yet identified in any gene (the heterogeneous group).

RESULTS

Age of onset was typically congenital among FLT4 mutation families and pubertal among FOXC2 mutation families, with similar male and female penetrance in both groups. Age of onset was highly variable in the families with no identified mutation, with substantially higher penetrance among female patients than male patients. In addition, male patients and female patients in the heterogeneous group had very different overall age of onset profiles.

CONCLUSIONS

The two genes identified to date that cause hereditary lymphedema have equal male and female effects, but each displays a different pattern of onset age and penetrance. The heterogeneous group represents a genetically heterogeneous population and has phenotypic overlaps with the FLT4 and FOXC2 mutation families.

摘要

目的

描述遗传性淋巴水肿的发病年龄模式和外显率,包括性别和基因异质性所导致的差异。

研究设计

对三个常染色体显性淋巴水肿家族队列进行Kaplan-Meier分析:(1)五个在FLT4基因有独特突变的家族;(2)十六个在FOXC2基因有独特突变的家族;(3)七十七个尚未在任何基因中鉴定出突变的家族(异质性组)。

结果

FLT4突变家族的发病年龄通常为先天性,FOXC2突变家族的发病年龄为青春期,两组中男性和女性的外显率相似。在未鉴定出突变的家族中,发病年龄高度可变,女性患者的外显率显著高于男性患者。此外,异质性组中的男性患者和女性患者的总体发病年龄概况非常不同。

结论

迄今为止确定的导致遗传性淋巴水肿的两个基因对男性和女性的影响相同,但每个基因都表现出不同的发病年龄模式和外显率。异质性组代表一个基因异质性群体,并且在表型上与FLT4和FOXC2突变家族有重叠。

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