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受发育性语言障碍影响的家族中,颞叶后区的脑回形态。

Gyral morphology in the posterior Sylvian region in families affected by developmental language disorder.

作者信息

Jackson T, Plante E

机构信息

Department of Biochemistry, University of Arizona, Tucson 85721, USA.

出版信息

Neuropsychol Rev. 1996 Jun;6(2):81-94. doi: 10.1007/BF01875369.

DOI:10.1007/BF01875369
PMID:8976499
Abstract

This study describes the family aggregation of gyral morphology in the posterior perisylvian region in families that contain one or more children with a developmental language disorder. The probands in these families were 8 male and 2 female children referred through therapy programs and schools for children with language and reading problems. Family members included both biological parents (10 m, 10 f) and all available siblings (6 m, 4 f). Gyral morphology in the members of these families was compared with control subjects (10 m, 10 f) who were without a personal or family history of developmental language disorders. Gyral morphology was evaluated using T1-weighted sagittal scans from a GE Signa 1.5T magnet, 5 mm consecutive slices through the full brain volume. A less common type of Sylvian fissure morphology was more frequently found in the hemispheres of language-disordered subjects and their first-degree relatives than in control subjects. In addition, the pattern of Sylvian fissure morphology across generations within the families suggests that this feature might be inherited from either parent. The elevated rate of extra gyri in the posterior perisylvian region in families affected by language disorder links an anomaly within a language-related brain region with familial risk for this disorder.

摘要

本研究描述了在有一个或多个患有发育性语言障碍儿童的家庭中,大脑外侧裂后区脑回形态的家族聚集性。这些家庭中的先证者是通过针对语言和阅读问题儿童的治疗项目及学校转诊而来的8名男童和2名女童。家庭成员包括亲生父母(10名男性,10名女性)以及所有在世的兄弟姐妹(6名男性,4名女性)。将这些家庭成员的脑回形态与无发育性语言障碍个人或家族史的对照受试者(10名男性,10名女性)进行比较。使用来自GE Signa 1.5T磁体的T1加权矢状面扫描评估脑回形态,对全脑体积进行5毫米连续切片。与对照受试者相比,在语言障碍受试者及其一级亲属的半球中更频繁地发现一种不太常见的外侧裂形态类型。此外,家庭中各代人外侧裂形态的模式表明,这一特征可能从父母任何一方遗传而来。受语言障碍影响的家庭中,大脑外侧裂后区额外脑回的发生率升高,这将一个与语言相关的脑区内的异常与该疾病的家族风险联系起来。

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