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Kallmann 综合征临床特征明确的患者的 CHD7 分析结果。

The results of CHD7 analysis in clinically well-characterized patients with Kallmann syndrome.

机构信息

Department of Genetics, University of Groningen, University Medical Center Groningen, 9700 RB Groningen, The Netherlands.

出版信息

J Clin Endocrinol Metab. 2012 May;97(5):E858-62. doi: 10.1210/jc.2011-2652. Epub 2012 Mar 7.

DOI:10.1210/jc.2011-2652
PMID:22399515
Abstract

CONTEXT

Kallmann syndrome (KS) and CHARGE syndrome are rare heritable disorders in which anosmia and hypogonadotropic hypogonadism co-occur. KS is genetically heterogeneous, and there are at least eight genes involved in its pathogenesis, whereas CHARGE syndrome is caused by autosomal dominant mutations in only one gene, the CHD7 gene. Two independent studies showed that CHD7 mutations can also be found in a minority of KS patients.

OBJECTIVE

We aimed to investigate whether CHD7 mutations can give rise to isolated KS or whether additional features of CHARGE syndrome always occur.

DESIGN

We performed CHD7 analysis in a cohort of 36 clinically well-characterized Dutch patients with KS but without mutations in KAL1 and with known status for the KS genes with incomplete penetrance, FGFR1, PROK2, PROKR2, and FGF8.

RESULTS

We identified three heterozygous CHD7 mutations. The CHD7-positive patients were carefully reexamined and were all found to have additional features of CHARGE syndrome.

CONCLUSION

The yield of CHD7 analysis in patients with isolated KS seems very low but increases when additional CHARGE features are present. Therefore, we recommend performing CHD7 analysis in KS patients who have at least two additional CHARGE features or semicircular canal anomalies. Identifying a CHD7 mutation has important clinical implications for the surveillance and genetic counseling of patients.

摘要

背景

卡尔曼综合征(KS)和 CHARGE 综合征是罕见的遗传性疾病,其特征为嗅觉缺失和促性腺激素低下性性腺功能减退同时发生。KS 在遗传学上具有异质性,至少有八个基因参与其发病机制,而 CHARGE 综合征仅由一个基因 CHD7 的常染色体显性突变引起。两项独立的研究表明,CHD7 突变也可在少数 KS 患者中发现。

目的

我们旨在研究 CHD7 突变是否可导致孤立性 KS,或者 CHARGE 综合征的其他特征是否总是存在。

设计

我们对 36 例临床特征明确的荷兰 KS 患者进行了 CHD7 分析,这些患者无 KAL1 基因突变,并且 KS 基因不完全外显,FGFR1、PROK2、PROKR2 和 FGF8 基因状态已知。

结果

我们发现了三个杂合 CHD7 突变。对 CHD7 阳性患者进行了仔细复查,发现他们均具有 CHARGE 综合征的其他特征。

结论

在孤立性 KS 患者中进行 CHD7 分析的检出率似乎非常低,但当存在其他 CHARGE 特征时,检出率会增加。因此,我们建议对至少有两个附加 CHARGE 特征或半规管异常的 KS 患者进行 CHD7 分析。确定 CHD7 突变对患者的监测和遗传咨询具有重要的临床意义。

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