ANO5突变导致颌骨长骨发育不良

doi:10.16352/j.issn.1001-6325.2024.11.1504

基础医学与临床 ›› 2024, Vol. 44 ›› Issue (11): 1504-1509.doi: 10.16352/j.issn.1001-6325.2024.11.1504

ANO5突变导致颌骨长骨发育不良

郑超群¹, 崔歌平¹, 任秀智^2*, 赵秀丽^1,2*

1.中国医学科学院基础医学研究所,北京协和医学院基础学院疑难重症及罕见病全国重点实验室医学遗传学系,北京 100005;
2.苏州大学附属儿童医院骨科,江苏苏州 215025

收稿日期:2024-05-14 修回日期:2024-07-03 出版日期:2024-11-05 发布日期:2024-10-31
通讯作者: ^*xiulizhao@ibms.pumc.edu.cn; renxiuzhi7320@suda.edu.cn
基金资助:
国家重点研发计划(2022YFC2703700);中国医学科学院医学与健康科技创新工程(2021-I2M-1-051)

Gnathodiaphyseal dysplasia caused by mutations in ANO5

ZHENG Chaoqun¹, CUI Geping¹, REN Xiuzhi^2*, ZHAO Xiuli^1,2*

1. Department of Medical Genetics, State Key Laboratory for Complex, Severe, and Rare Diseases, Institute of Basic Medical Sciences CAMS, School of Basic Medicine PUMC, Beijing 100005;
2. Pediatric Orthopedics, Children's Hospital of Soochow University, Suzhou 215025, China

Received:2024-05-14 Revised:2024-07-03 Online:2024-11-05 Published:2024-10-31
Contact: ^*xiulizhao@ibms.pumc.edu.cn; renxiuzhi7320@suda.edu.cn

摘要/Abstract

摘要： 目的在两个颌骨长骨发育不良(GDD)家系中进行临床特征和致病基因变异鉴定。方法对先证者及其家系成员进行面部和四肢外观畸形骨骼形态的观察,采集先证者及其父母的周静脉外周血3~4 mL;采用常规酚-氯仿法提取外周血基因组DNA;通过全外显子组测序(WES)对先证者进行候选致病基因变异的筛查,再经PCR-Sanger测序在先证者及其家系成员中针对候选致病变异进行变异验证;通过致病变异的家系共分离、变异位点进化保守性、候选致病变异的群体等位基因频率和生物信息学分析进行候选致病变异的致病性鉴定,最终确定上述家系GDD患者的致病变异。结果在两个GDD先证者中均鉴定到ANO5的杂合错义变异。家系1致病变异为位于ANO5第11外显子的c.1 066T＞G,家系2致病变异为位于ANO5第15外显子的c.1 553G＞A。上述两个变异分别导致ANO5编码蛋白第356位氨基酸由半胱氨酸变为甘氨酸(p.Cys356Gly),及第518氨基酸由甘氨酸变为谷氨酸(p.Gly518Glu)。结论本研究首次在中国人群中发现了c.1 066T＞G(p.Cys356Gly)致病变异,为患者疾病进展预后和未来产前基因诊断提供了重要依据。

关键词: 颌骨长骨发育不良, 全外显子组测序, ANO5, 变异

Abstract: Objective To identify the clinical features and pathogenic variants in two unrelated families with gnathodiaphyseal dysplasia (GDD), a rare genetic bone disorder. Methods Facial and limb deformities and skeletal morphology were observed in the probands and their family members. Peripheral blood samples (3-4 mL) were collected from the probands and their parents. Genomic DNA was extracted by standard phenol-chloroform method. Whole exome sequencing (WES) was performed to screen for candidate pathogenic gene variants of the probands. PCR-Sanger sequencing was used to validate the candidate pathogenic variants in the probands and their family members. The pathogenic variants responsible for GDD in the target families were determined through co-segregation of the pathogenic variants in the affected families, evolutionary conservation at the mutation sites,population allele frequency analysis and bioinformatics analysis. Results Heterozygous missense variants in the ANO5 gene were identified in both GDD probands. In family 1, the pathogenic variant was c.1 066T＞G located in the exon 11 of the ANO5 gene, while in family 2, the pathogenic variant was c.1 553G＞A located in the exon 15 of the ANO5. These two variants resulted in the substitutions of amino acid cysteine with glycine at position 356 (p.Cys356Gly) and amino acid glycine with glutamic acid at position 518 (p.Gly518Glu) in the ANO5 protein, respectively. Conclusions This study first identified the pathogenic variant c.1 066T＞G (p.Cys356Gly) in Chinese population, provided important evidence for prediction of disease prognosis and development of potential prenatal genetic diagnosis.

Key words: gnathodiaphyseal dysplasia, whole exome sequencing, ANO5, variants

中图分类号:

310.27

郑超群, 崔歌平, 任秀智, 赵秀丽. ANO5突变导致颌骨长骨发育不良[J]. 基础医学与临床, 2024, 44(11): 1504-1509.

ZHENG Chaoqun, CUI Geping, REN Xiuzhi, ZHAO Xiuli. Gnathodiaphyseal dysplasia caused by mutations in ANO5[J]. Basic & Clinical Medicine, 2024, 44(11): 1504-1509.

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ANO5突变导致颌骨长骨发育不良

Gnathodiaphyseal dysplasia caused by mutations in ANO5

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