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TUBB 相关疾病的临床变异性:通过重新分析进行诊断。

Clinical variability of TUBB-associated disorders: Diagnosis through reanalysis.

机构信息

Center for Applied Genomics, The Children's Hospital of Philadelphia, Philadelphia, Pennsylvania, USA.

Division of Human Genetics, The Children's Hospital of Philadelphia, Philadelphia, Pennsylvania, USA.

出版信息

Am J Med Genet A. 2020 Dec;182(12):3035-3039. doi: 10.1002/ajmg.a.61897. Epub 2020 Oct 5.

Abstract

A range of clinical findings have been associated with heterozygous mutations in the Beta Tubulin (TUBB) gene, including microcephaly, structural brain abnormalities, intellectual disability, and skin creases. We report a 5-year-old male who presented for evaluation of cleft palate, cardiac defects, growth retardation, hemivertebrae causing scoliosis, and preauricular skin tags. Previous clinical exome sequencing of this patient was nondiagnostic, but reanalysis in the research setting identified a de novo missense c. 925C>G p.(Arg309Gly) mutation in TUBB. This mutation was not found in population allele frequency databases, and was classified to be likely pathogenic. This patient shares some phenotypic characteristics with previous reported patients of TUBB mutations of the two TUBB-related phenotypes: "Cortical dysplasia, complex, with other brain malformations 6" [MIM 615771] and "Circumferential Skin Creases Kunze type (CSC-KT)" [MIM 156610], but has no excess skin creases or structural brain anomalies. We also report previously undescribed features, including transposition of the great arteries and vertebral fusion, thus representing phenotype expansion of TUBB-associated disorders.

摘要

一系列临床发现与 Beta 微管蛋白(TUBB)基因的杂合突变有关,包括小头畸形、结构性脑异常、智力障碍和皮肤折痕。我们报告了一名 5 岁男性,他因腭裂、心脏缺陷、生长迟缓、半椎体引起的脊柱侧凸和耳前皮肤标签就诊。该患者先前的临床外显子组测序无诊断意义,但在研究环境中的重新分析确定了 TUBB 中存在一个新的错义 c.925C>G p.(Arg309Gly)突变。该突变未在人群等位基因频率数据库中发现,被归类为可能致病。该患者与先前报道的 TUBB 突变的两个 TUBB 相关表型的一些表型特征相吻合:“皮质发育不良,伴有其他脑畸形 6”[MIM 615771]和“环状皮肤皱褶 Kunze 型(CSC-KT)”[MIM 156610],但没有过多的皮肤折痕或结构性脑异常。我们还报告了以前未描述的特征,包括大动脉转位和椎体融合,因此代表了 TUBB 相关疾病的表型扩展。

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