对疑似患有I型斯-韦二氏综合征的伊朗患者中常见COL2A1基因变异的评估。
Evaluation of common COL2A1 gene variants in Iranian patients suspected with Stickler syndrome type I.
作者信息
Abolhasani Fatemeh, Abdali Hossein, Kazemi Mohammad, Attar Bijan Movahedian, Derakhshandeh Fatemeh, Hosseinzadeh Majid
机构信息
Department of Genetics and Molecular Biology, School of Medicine, Isfahan University of Medical Sciences, Isfahan, Iran.
Department of Surgery, School of Medicine, Plastic and Reconstructive Surgery, Craniofacial and Cleft Research Center, Isfahan University of Medical Sciences, Isfahan, Iran.
出版信息
J Res Med Sci. 2025 Jan 30;30:6. doi: 10.4103/jrms.jrms_447_24. eCollection 2025.
BACKGROUND
Stickler syndrome, also known as hereditary progressive arthro-ophthalmopathy, is a connective tissue disorder that arises from mutations in multiple genes, each with distinct hereditary patterns. Stickler syndrome type I, which is inherited in an autosomal dominant manner, is specifically linked to mutations in the gene. The objective of this study is to investigate the prevalence of common variants of the gene among individuals suspected of having Stickler syndrome type I.
MATERIALS AND METHODS
Twenty-six Iranian patients suspected of having Stickler syndrome type I referring to Al-Zahra Hospital of Isfahan were employed in this cross-sectional study. The DNA was extracted from the patient's peripheral blood samples, and the selected exons of the gene were amplified by polymerase chain reaction. Subsequently, the purified amplicons were subjected to Sanger sequencing to identify common variants associated with Stickler syndrome type I.
RESULTS
All patients exhibit cleft abnormalities (palate, lip, and alveolar), 84.6% of patients exhibit ocular abnormalities, 53.8% of patients exhibit hearing abnormalities, and 34.6% of patients exhibit skeletal abnormalities. As the data displays, the highest phenotype presentation prevalence rate was related to cleft lip and palate, while hemiparesis was the lowest clinical finding among the patients. Molecular analysis which conducted to screen the gene of patients, identified two different variants, including a novel nonsense variant, (c.1030C>T), consistent with dominantly inherited Stickler syndrome type I, also synonymous mutation (c.213C>T) affecting in exon 2, which have been reported in database.
CONCLUSION
Genetic analysis of Twenty-six unrelated families with Stickler syndrome type I disorder discovered one novel pathogenic variant in the gene in a patient with Stickler syndrome type I. Genetic analysis is helpful for the diagnosis of this clinically variable and genetically heterogeneous disorder.
背景
斯迪克勒综合征,也称为遗传性进行性关节眼病,是一种结缔组织疾病,由多个基因的突变引起,每个基因都有不同的遗传模式。I型斯迪克勒综合征以常染色体显性方式遗传,与该基因的突变有特定关联。本研究的目的是调查疑似I型斯迪克勒综合征患者中该基因常见变异的患病率。
材料与方法
本横断面研究纳入了26名转诊至伊斯法罕的阿尔-扎赫拉医院的疑似I型斯迪克勒综合征的伊朗患者。从患者外周血样本中提取DNA,通过聚合酶链反应扩增该基因的选定外显子。随后,对纯化的扩增子进行桑格测序,以鉴定与I型斯迪克勒综合征相关的常见变异。
结果
所有患者均表现出腭裂异常(腭、唇和牙槽),84.6%的患者表现出眼部异常,53.8%的患者表现出听力异常,34.6%的患者表现出骨骼异常。如数据所示,最高的表型表现患病率与唇腭裂有关,而偏瘫是患者中最低的临床发现。对患者该基因进行筛查的分子分析确定了两个不同的变异,包括一个新的无义变异(c.1030C>T),与显性遗传的I型斯迪克勒综合征一致,还有一个影响外显子2的同义突变(c.213C>T),该突变已在数据库中报道。
结论
对26个患有I型斯迪克勒综合征的无关家族进行的基因分析在一名I型斯迪克勒综合征患者的该基因中发现了一个新的致病变异。基因分析有助于诊断这种临床可变且基因异质性的疾病。
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