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右心室双出口:病因及关联

Double outlet right ventricle: aetiologies and associations.

作者信息

Obler D, Juraszek A L, Smoot L B, Natowicz M R

机构信息

Department of Cardiology, Children's Hospital, Boston, MA 02115, USA.

出版信息

J Med Genet. 2008 Aug;45(8):481-97. doi: 10.1136/jmg.2008.057984. Epub 2008 May 2.

DOI:10.1136/jmg.2008.057984
PMID:18456715
Abstract

BACKGROUND

Double outlet right ventricle (DORV), a clinically significant congenital heart defect, occurs in 1-3% of individuals with congenital heart defects. In contrast to other major congenital heart defects, there are no systematic or comprehensive data regarding associations, aetiologies, and pathogenesis of DORV. We analysed reported cases in the medical literature to address these issues.

METHODS

We queried the PubMed database using key words "double outlet right ventricle" and "DORV" for case reports, epidemiologic analyses and animal studies with this cardiac anomaly. The anatomic subtype of DORV was classified according to criteria of Van Praagh.

RESULTS

Chromosomal abnormalities were present in 61 of the 149 cases of DORV. Trisomies 13 and 18, and del 22q11 were the most commonly associated cytogenetic lesions; different anatomic subtypes of DORV were noted in trisomies 13 and 18 versus del 22q11. DORV was reported in many uncommon or rare non-chromosomal syndromes. Mutations and non-synonymous sequence variants in the CFC1 and CSX genes were the most commonly reported monogenic loci associated with DORV in humans; numerous genes are reported in murine models of DORV. Animal studies implicate maternal diabetes and prenatal exposure to ethanol, retinoids, theophylline, and valproate in DORV teratogenesis.

CONCLUSIONS

The large number of genes associated with DORV in both humans and animal models and the different anatomic subtypes seen in specific aetiologies indicate the likelihood of several distinct pathogenetic mechanisms for DORV, including impairment of neural crest derivative migration and impairment of normal cardiac situs and looping.

摘要

背景

双出口右心室(DORV)是一种具有临床意义的先天性心脏缺陷,在先天性心脏缺陷患者中发生率为1% - 3%。与其他主要先天性心脏缺陷不同,目前尚无关于DORV的关联、病因及发病机制的系统或全面数据。我们分析了医学文献中报道的病例以解决这些问题。

方法

我们使用关键词“双出口右心室”和“DORV”在PubMed数据库中查询有关该心脏异常的病例报告、流行病学分析及动物研究。DORV的解剖亚型根据Van Praagh标准进行分类。

结果

149例DORV病例中有61例存在染色体异常。13三体、18三体及22q11缺失是最常见的相关细胞遗传学病变;13三体和18三体与22q11缺失所见的DORV解剖亚型不同。DORV在许多不常见或罕见的非染色体综合征中也有报道。CFC1和CSX基因的突变及非同义序列变异是人类中最常报道的与DORV相关的单基因位点;在DORV的小鼠模型中报道了众多基因。动物研究表明母体糖尿病以及孕期暴露于乙醇、视黄酸、茶碱和丙戊酸与DORV致畸有关。

结论

在人类和动物模型中与DORV相关的大量基因以及特定病因中所见的不同解剖亚型表明,DORV可能存在几种不同的发病机制,包括神经嵴衍生物迁移受损以及正常心脏位置和环化受损。

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Double outlet right ventricle: aetiologies and associations.右心室双出口:病因及关联
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