Ding Xianhong, Chen Hongliang, Lu Yang, Xu Mengyi, Hu Bingjie, Fang Yicheng, Shen Bo
Department of Laboratory, Taizhou Hospital of Zhejiang Province, Taizhou, Zhejiang 318050, China.
Zhonghua Yi Xue Yi Chuan Xue Za Zhi. 2025 Jan 10;42(1):41-50. doi: 10.3760/cma.j.cn511374-20240828-00459.
To determine the types of genetic variants in six Chinese pedigrees affected with Marfan syndrome (MFS) and analyze their clinical characteristics and molecular pathogenesis.
Six MFS pedigrees presented at the Taizhou Enze Medical Center (Group) between 2017 and 2022 were selected as the study subjects. Clinical data of pedigrees were retrospectively analyzed. Peripheral blood samples were collected from the probands and their family members for the extraction of genomic DNA. Whole exome sequencing (WES) was carried out. Candidate variants of the FBN1 gene were verified by Sanger sequencing. Based on the guidelines from the American College of Medical Genetics and Genomics (ACMG), pathogenicity of the candidate variants was assessed. AlphaFold3 and PyMOL software were used for homology modeling of the FBN1 protein and analysis of its three-dimensional structure and amino acid sequence conservation. This study was approved by the Medical Ethics Committee of Taizhou Enze Medical Center (Group) (Ethics No. 20231002).
Cardiovascular system abnormalities were noted in all pedigrees, ocular abnormalities were present in pedigrees 2 and 5, skeletal system abnormalities were presented in pedigrees 1, and 4 to 6. FBN1 gene mutations were identified in all pedigrees, including c.1957_1958dupGT (p.Asp654fs), c.5014T>A (p.Cys1672Ser), c.8135delC (p.Pro2712fs), c.2302G>T (p.Glu768*), c.3473A>G (p.Glu1158Gly) and c.6169C>T (p.Arg2057*), with each involving a different exon. Four variants were rated as pathogenic, one as likely pathogenic, and one as variant of uncertain significance. Among these, c.5014T>A (p.Cys1672Ser), c.1957_1958dupGT (p.Asp654fs), c.8135delC (p.Pro2712fs), and c.2302G>T (p.Glu768*) were unreported previously. Bioinformatic analysis with SIFT and PolyPhen-2 predicted that the c.5014T>A (p.Cys1672Ser) and c.3473A>G (p.Glu1158Gly) variants were deleterious. Protein homologous sequence alignment analysis revealed that the four novel mutation sites are highly conserved across various species. Homology modeling of the FBN1 protein three-dimensional structure indicated that the six variant sites in the amino acid sequence are all close to hydrogen bonds and may alter the secondary and tertiary structures to varying degrees, thereby confirmed the relationship between the variants and MFS.
Four novel variants of the FBN1 gene have been discovered in this study, which has enriched the mutational and phenotypic spectrum of MFS and provided a basis for disease diagnosis and genetic counseling.
确定六个患有马凡综合征(MFS)的中国家系中的基因变异类型,并分析其临床特征和分子发病机制。
选取2017年至2022年期间在台州恩泽医疗中心(集团)就诊的六个MFS家系作为研究对象。对家系的临床资料进行回顾性分析。采集先证者及其家庭成员的外周血样本用于提取基因组DNA。进行全外显子组测序(WES)。通过Sanger测序验证FBN1基因的候选变异。根据美国医学遗传学与基因组学学会(ACMG)的指南评估候选变异的致病性。使用AlphaFold3和PyMOL软件对FBN1蛋白进行同源建模,并分析其三维结构和氨基酸序列保守性。本研究获得台州恩泽医疗中心(集团)医学伦理委员会批准(伦理编号:20231002)。
所有家系均有心血管系统异常,家系2和5有眼部异常,家系1以及4至6有骨骼系统异常。所有家系均鉴定出FBN1基因突变,包括c.1957_1958dupGT(p.Asp654fs)、c.5014T>A(p.Cys1672Ser)、c.8135delC(p.Pro2712fs)、c.2302G>T(p.Glu768*)、c.3473A>G(p.Glu1158Gly)和c.6169C>T(p.Arg2057*),每个突变涉及不同的外显子。四个变异被评为致病性,一个为可能致病性,一个为意义未明的变异。其中,c.5014T>A(p.Cys1672Ser)、c.1957_1958dupGT(p.Asp654fs)、c.8135delC(p.Pro2712fs)和c.2302G>T(p.Glu768*)此前未被报道。使用SIFT和PolyPhen-2进行的生物信息学分析预测,c.5014T>A(p.Cys1672Ser)和c.3473A>G(p.Glu1158Gly)变异有害。蛋白质同源序列比对分析显示,四个新的突变位点在不同物种中高度保守。FBN1蛋白三维结构的同源建模表明,氨基酸序列中的六个变异位点均靠近氢键,可能不同程度地改变二级和三级结构,从而证实了变异与MFS之间的关系。
本研究发现了四个FBN1基因的新变异,丰富了MFS的突变和表型谱,为疾病诊断和遗传咨询提供了依据。
