与卡尼复合征变异型相关的围产期肌球蛋白重链突变。

Mutation of perinatal myosin heavy chain associated with a Carney complex variant.

作者信息

Veugelers Mark, Bressan Michael, McDermott Deborah A, Weremowicz Stanislawa, Morton Cynthia C, Mabry C Charlton, Lefaivre Jean-François, Zunamon Alan, Destree Anne, Chaudron Jean-Marie, Basson Craig T

机构信息

Molecular Cardiology Laboratory, Greenberg Cardiology Division, Department of Medicine, Weill Medical College of Cornell University, New York 10021, USA.

出版信息

N Engl J Med. 2004 Jul 29;351(5):460-9. doi: 10.1056/NEJMoa040584.

DOI:10.1056/NEJMoa040584

PMID:15282353

Abstract

BACKGROUND

Familial cardiac myxomas occur in the hereditary syndrome Carney complex. Although PRKAR1A mutations can cause the Carney complex, the disorder is genetically heterogeneous. To identify the cause of a Carney complex variant associated with distal arthrogryposis (the trismus-pseudocamptodactyly syndrome), we performed clinical and genetic studies.

METHODS

A large family with familial cardiac myxomas and the trismus-pseudocamptodactyly syndrome (Family 1) was identified and clinically evaluated along with two families with trismus and pseudocamptodactyly. Genetic linkage analyses were performed with the use of microsatellite polymorphisms to determine a locus for this Carney complex variant. Positional cloning and mutational analyses of candidate genes were performed to identify the genetic cause of disease in the family with the Carney complex as well as in the families with the trismus-pseudocamptodactyly syndrome.

RESULTS

Clinical evaluations demonstrated that the Carney complex cosegregated with the trismus-pseudocamptodactyly syndrome in Family 1, and genetic analyses demonstrated linkage of the disease to chromosome 17p12-p13.1 (maximum multipoint lod score, 4.39). Sequence analysis revealed a missense mutation (Arg674Gln) in the perinatal myosin heavy-chain gene (MYH8). The same mutation was also found in the two families with the trismus-pseudocamptodactyly syndrome. Arg674 is highly conserved evolutionarily, localizes to the actin-binding domain of the perinatal myosin head, and is close to the ATP-binding site. We identified nonsynonymous MYH8 polymorphisms in patients with cardiac myxoma syndromes but without arthrogryposis.

CONCLUSIONS

We describe a novel heart-hand syndrome involving familial cardiac myxomas and distal arthrogryposis and demonstrate that these disorders are caused by a founder mutation in the MYH8 gene. Our findings demonstrate novel roles for perinatal myosin in both the development of skeletal muscle and cardiac tumorigenesis.

摘要

背景

家族性心脏黏液瘤发生于遗传性综合征卡尼综合征。虽然PRKAR1A基因突变可导致卡尼综合征，但该疾病在基因上具有异质性。为了确定与远端关节挛缩症（牙关紧闭-假性并指综合征）相关的卡尼综合征变异型的病因，我们进行了临床和遗传学研究。

方法

识别出一个患有家族性心脏黏液瘤和牙关紧闭-假性并指综合征的大家庭（家系1），并对其进行临床评估，同时评估另外两个患有牙关紧闭和假性并指的家系。使用微卫星多态性进行遗传连锁分析，以确定这种卡尼综合征变异型的基因座。对候选基因进行定位克隆和突变分析，以确定患有卡尼综合征的家系以及患有牙关紧闭-假性并指综合征的家系中的疾病遗传病因。

结果

临床评估表明，家系1中卡尼综合征与牙关紧闭-假性并指综合征共分离，遗传分析表明该疾病与17号染色体p12-p13.1区域连锁（最大多点对数优势分数为4.39）。序列分析显示围产期肌球蛋白重链基因（MYH8）存在一个错义突变（Arg674Gln）。在另外两个患有牙关紧闭-假性并指综合征的家系中也发现了相同的突变。Arg674在进化上高度保守，定位于围产期肌球蛋白头部的肌动蛋白结合结构域，且靠近ATP结合位点。我们在患有心脏黏液瘤综合征但无关节挛缩症的患者中鉴定出非同义MYH8多态性。