Your search keyword '"Fibrillin-1 genetics"' showing total 11 results

1. [Correlation of posterior segment lesions with anterior segment biometric parameters and FBN1 genotype in patients with Marfan syndrome].

Author

Liu Y, Chen TH, and Jiang YX

Subjects

Adolescent, Child, Female, Humans, Male, Young Adult, Adipokines, Anterior Eye Segment, Biometry, Cross-Sectional Studies, Macular Degeneration genetics, Mutation, Posterior Eye Segment pathology, Infant, Newborn, Infant, Child, Preschool, Fibrillin-1 genetics, Genotype, Marfan Syndrome genetics

Abstract

Objective: To investigate the characteristics of posterior segment lesions in Marfan syndrome (MFS) patients and their relationship with anterior segment biometric parameters and FBN1 genotype. Methods: A cross-sectional study was conducted. A total of 121 MFS patients, 76 males and 45 females, with an average age of (11.72±11.66) years, who visited the Department of Ophthalmology, Eye & ENT Hospital of Fudan University from January 2013 to March 2023 were included. The presence of posterior scleral staphyloma was observed using B-mode ultrasound, and macular lesions were identified and classified using the atrophy-traction-neovascularization system based on ultra-widefield fundus images, color fundus images, and optical coherence tomography scans. Anterior segment biometric parameters, including axial length of the eye, average corneal curvature, corneal astigmatism, horizontal corneal diameter, anterior chamber depth, and lens thickness, were collected, and the direction and extent of lens dislocation were observed. Molecular genetic analysis of FBN1 gene mutations in patients was performed using next-generation sequencing based on a panel of ocular genetic diseases, and the impact of the genotype and anterior segment biometric parameters on the posterior segment manifestations was analyzed. Results: Sixty patients exhibited posterior segment lesions, including retinal detachment (4 cases, 3.31%), macular lesions (47 cases, 38.84%), and posterior scleral staphyloma (54 cases, 44.63%). There was statistically significant difference in axial length of the eye between patients with and without posterior scleral staphyloma [23.09 (22.24, 24.43) and 27.04 (25.44, 28.88) mm], between patients with and without macular lesions [23.16 (22.24, 24.61) and 27.04 (25.74, 28.78) mm], and between patients with and without atrophic macular lesions [23.16 (22.24, 24.61) and 27.04 (25.74, 28.79) mm] (all P <0.001). There was statistically significant difference in anterior chamber depth between patients with and without macular lesions [3.11 (2.75, 3.30) and 3.34 (3.09, 3.60) mm] ( P <0.05). There was also statistically significant difference in corneal astigmatism between patients with and without posterior scleral staphyloma [2.15 (1.20, 2.93) and 1.40 (1.00, 2.20) diopters] ( P <0.05). The location and region of the FBN1 gene mutation not only showed statistically significant difference from the positive rates of posterior scleral staphyloma and macular lesions (all P <0.05), but also influenced the occurrence of atrophic macular lesions (both P <0.05). Patients with FBN1 mutations located in the transforming growth factor β regulatory sequence had the highest proportion of posterior scleral staphyloma and macular lesions (both 10/11). Conclusions: Posterior scleral staphyloma and macular lesions have a relatively high incidence in MFS patients and tend to progress to more severe grades. The age, axial length of the eye, anterior chamber depth, corneal astigmatism, and location and region of the FBN1 gene mutation are factors affecting the posterior segment lesions in MFS patients.

Published

2024

2. [Clinical phenotype and genetic analysis of six Chinese patients affected with Acromicric dysplasia due to variants of FBN1 gene].

Author

Yu M, Liu X, Ran N, Yang Z, and Shan Y

Subjects

Humans, Female, Animals, Retrospective Studies, Phenotype, China, Fibrillin-1 genetics, Adipokines, Limb Deformities, Congenital, Dwarfism, Bone Diseases, Developmental

Abstract

Objective: To retrospectively analyze the clinical and genetic characteristics of six patients with Acromicric dysplasia due to variants of the FBN1 gene., Methods: Six patients who had visited the Affiliated Hospital of Qingdao University between February 2018 and October 2020 were selected as the study subjects. Clinical data of the patients were collected. High-throughput sequencing was carried out. And candidate variants were verified by Sanger sequencing., Results: All of the six patients had presented with severe short stature (< 3s), brachydactyly, short and broad hands and feet. Other manifestations included joint stiffness, facial dysmorphism, delayed bone age, liver enlargement, coracoid femoral head, and lumbar lordosis. Genetic testing revealed that all had harbored heterozygous variants of the FBN1 gene. Patient 1 had harbored a c.5183C>T (p.A1728V) missense variant in exon 42, which had derived from his father (patient 2). Patient 3 had harbored a c.5284G>A (p.G1762S) missense variant in exon 43, which had derived from her mother (patient 4). Patient 5 had harbored a c.5156G>T (p.C1719F) missense variant in exon 42, which was de novo in origin. Patient 6 had harbored a c.5272G>T (p.D1758Y) missense variant in exon 43, which was also de novo in origin. The variants carried by patients 1, 3 and 6 were known to be pathogenic. Based on the guidelines from the American College of Medical Genetics and Genomics (ACMG), the FBN1: c.5156G>T was rated as a pathogenic variant (PS2+PM1+PM2&#95;Supporting +PM5+PP3)., Conclusion: All of the six patients had severe short stature and a variety of other clinical manifestations, which may be attributed to the variants of the FBN1 gene.

Published

2024

3. [Clinical manifestations and genetic analysis of 4 patients with variants of FBN1 gene].

Author

Liu X, Yang M, Xie H, Zhao Q, Xu B, Xiao X, Tan Y, and Liu S

Subjects

Female, Pregnancy, Humans, Male, Exons, China, Genetic Counseling, Genetic Testing, Mutation, Fibrillin-1 genetics, Family, Marfan Syndrome genetics

Abstract

Objective: To explore the genetic basis for four patients suspected for Marfan syndrome (MFS)., Methods: Four male patients with suspected MFS and their family members who were treated at West China Second Hospital of Sichuan University from September 12, 2019 to March 27, 2021 were selected as the study subjects. Peripheral venous blood samples were collected from the patients and their parents or other pedigree members for the extraction of genomic DNA. Whole exome sequencing was carried out, and candidate variants were validated by Sanger sequencing. The pathogenicity of the variants was determined based on the guidelines from the American College of Medical Genetics and Genomics (ACMG)., Results: Genetic testing revealed that all four patients have harbored variants of the FBN1 gene, including c.430&#95;433del (p.His144fs) deletional variant in exon 5, c.493C>T (p.Arg165*) nonsense variant in exon 6, c.5304&#95;5306del (p.Asp1768del) deletional variant in exon 44 and c.5165C>G (p.Ser1722Cys) missense variant in exon 42. According to the ACMG guidelines, the c.430&#95;433del and c.493C>T were classified as pathogenic variants (PVS1+PM2&#95;Supporting+PP4; PVS1+PS1+PS2+PM2&#95;Supporting+PP4). c.5304&#95;5306del and c.5165C>G were classified as likely pathogenic variants (PS2+PM2&#95;Supporting+PM4+PP4; PS2&#95;Moderate+PS1+PM1+PM2&#95;Supporting)., Conclusion: The c.430&#95;433del and c.5304&#95;5306del variants of the FBN1 gene identified in this study were unreported previously. Above results have enriched the variation spectrum of the FBN1 gene and provided a basis for genetic counseling and prenatal diagnosis of patients with MFS and acromicric dysplasia.

Published

2023

4. [Analysis of a child with Marfan syndrome due to a novel variant of FBN1 gene].

Author

Zhao L, Liu S, Hu W, and Jin P

Subjects

Male, Humans, Fibrillin-1 genetics, Mutation, Genotype, Genetic Association Studies, Marfan Syndrome genetics

Abstract

Objective: To carry out genetic testing for a child with Marfan syndrome (MFS) and explore its genotype-phenotype correlation., Methods: Peripheral blood samples of the child and his parents were collected for the extraction of genomic DNA and subjected to whole exome sequencing (WES). Candidate variants were verified by Sanger sequencing. Functional impact of the variant was predicted by using bioinformatic software., Results: The child, a 13-year-old male, has featured Marfanoid habitus, with arm span exceeding his height, tapering fingers and toes, pectus excavatum and scoliosis, but absence of typical cardiovascular system diseases such as aortic dilation, thoracic-abdominal aortic aneurysm, mitral valve prolapse, and lens dislocation. The child has harbored a novel splice site variant c.7383&#95;7413del (p. N2461Kfs*211) of the FBN1 gene, which was not found in his parents and younger brother. The variant was unreported previously., Conclusion: The novel variant of p. N2461Kfs*211 of the FBN1 gene probably underlay the MFS in this child. Above finding has enriched the genotypic and phenotypic spectrum of MFS.

Published

2023

5. [Analysis of FBN1 genemutations in a pedigree with Marfan syndrome].

Author

Zheng Q, Li KL, Dai GL, Xiong D, Yao MY, Chen X, Li YM, Zhang YY, Li HR, and Cao Y

Subjects

Exons, Fibrillin-1 genetics, Humans, Mutation, Missense, Pedigree, Marfan Syndrome diagnosis, Marfan Syndrome genetics, Marfan Syndrome pathology

Abstract

Mutations in fibrillin-1 (FBN1) were detected in an autosomal dominant Marfan syndrome (MFS) pedigree. The related phenotypes and the significance of mutation screening were discussed. Complete medical and cardiovascular examinations for all pedigree members were performed. Whole exons sequencing (WES) was used to sequence the DNA of the patients and their relatives. The potential pathogenic mutation sites were screened by bioinformatics method. Sanger sequencing was used to verify the mutation sites in the pedigree. The results showed that FBN1 missense mutation was c.6806 T>C in exon 56, resulting in isoleucine being replaced by threonine (p. Ile2269Thr). This mutation has not been reported in Chinese Han population. The occurrence of the mutations strongly correlated with the phenotypes of the patients. The results expand the mutation spectrum of FBN1, and it is helpful to further explore the molecular pathogenesis of MFS and MFS related diseases.

Published

2022

6. [Latest advances in the diagnosis and treatment of Marfan syndrome].

Author

Yang ST and Luo F

Subjects

Fibrillin-1 genetics, Humans, Infant, Newborn, Mutation, Marfan Syndrome diagnosis, Marfan Syndrome genetics, Marfan Syndrome therapy

Abstract

Marfan syndrome (MFS) is a multisystem connective tissue disease with autosomal dominant inheritance. It is mainly caused by FBN1 gene mutation and often has different clinical manifestations. Neonatal MFS is especially rare with severe conditions and a poor prognosis. At present, there is still no radical treatment method for MFS, but early identification, early diagnosis, and early treatment can effectively prolong the life span of patients. This article reviews the latest advances in the diagnosis and treatment of MFS.

Published

2022

7. [A de novo mutation leading to Marfan syndrome in a case].

Author

Liang S, Liu L, Qiu X, and Liu J

Subjects

Child, Exons, Humans, Mutation, Sequence Deletion, Exome Sequencing, Fibrillin-1 genetics, Heart Defects, Congenital, Marfan Syndrome genetics

Abstract

Objective: To explore the genetic basis for a child featuring unexplained rapid growth and heart malformation., Methods: Whole exome sequencing (WES)was carried out for the patient. Suspected variant was verified by Sanger sequencing and subjected to bioinformatic analysis., Results: The child was found to harbor a novel de novo c.5846&#95;5848delATA (p. N1949del) variant in exon 48 of the FBN1 gene, which was predicted to be pathogenic by Mutation Taster. The patient was ultimately diagnosed with Marfan syndrome., Conclusion: Above finding has enriched the spectrum of genetic variants associated with Marfan syndrome. WES has provided a powerful tool for the diagnosis of rare diseases.

Published

2021

8. [Identification of a novel FBN1 variant in a pedigree affected with Marfan syndrome].

Author

Rong J, Dong S, Wang C, He S, Luo J, Li M, Deng Q, and Yan M

Subjects

DNA Mutational Analysis, Exons, Fibrillins, Humans, Mutation, Pedigree, Fibrillin-1 genetics, Marfan Syndrome genetics, Mutation, Missense

Abstract

Objective: To explore the genetic basis for a pedigree affected with Marfan syndrome (MFS)., Methods: Clinical data of the patients was collected. With genomic DNA extracted from peripheral blood samples, potential mutation was detected by targeted exome sequencing. Candidate variants were validated by Sanger sequencing and bioinformatic analysis., Results: Targeted exome sequencing and Sanger sequencing revealed a missense c.649T to C(p.Trp217Arg) variant in the exon 7 of FBN1 gene, which was unreported previously. Bioinformatics analysis suggested that the variant can cause amino acid replacement and affect the structure and function of fibrillin-1., Conclusion: A novel missense variant of the FBN1 gene was identified, which probably underlies the autosomal dominant MFS in this pedigree.

Published

2019

9. [Analysis of FBN1 gene mutations in two pedigrees affected with Marfan syndrome].

Author

Yang L, Guo X, Jiang L, Gong B, and Qu C

Subjects

DNA Mutational Analysis, Exons, Fibrillins, Humans, Mutation, Pedigree, Fibrillin-1 genetics, Marfan Syndrome genetics

Abstract

Objective: To detect mutations of fibrillin-1 (FBN1) gene in two pedigrees affected with Marfan syndrome (MFS)., Wethods: Peripheral blood samples were collected from MFS patients and their healthy family members for extracting genomic DNA. All of the 65 exons of the FBN1 gene were analyzed by next-generation sequencing. PolyPhen-2 and SIFT was used to predict structural and functional changes in FBN1 protein., Results: Patients from both pedigrees presented ocular and skeletal manifestations suggestive of MFS. Two novel heterozygous mutations of the FBN1 gene, including c.1879C>T (p.R627C) in exon 16 and c.2584T>C (p.C862R) in exon 22, were identified. The same mutations were not found among unaffected members. By bioinformatic analysis, the mutations may affect the structure and function of the FBN1 protein., Conclusion: The c.1879C>T and c.2584T>C mutations of the FBN1 gene probably account for the disease in the two pedigrees, respectively. Identification of the c.2584T>C has enriched the spectrum of FBN1 gene mutations.

Published

2019

10. [Mutation analysis of FBN1 gene in a child with Marfan syndrome].

Author

Jiang L, Zhang D, Xiao Y, Wang Q, Gong B, Guo X, Huang M, and Yang Z

Subjects

Amino Acid Sequence, Base Sequence, Child, DNA Mutational Analysis, Fibrillin-1 chemistry, Humans, Male, Molecular Sequence Data, Sequence Alignment, Fibrillin-1 genetics, Marfan Syndrome genetics

Abstract

Objective: To detect potential mutations of fibrillin-1 (FBN1) gene in a child with Marfan syndrome (MFS) and explore its molecular pathogenesis., Methods: The 66 exons of the FBN1 gene were analyzed by direct sequencing. SIFT and PolyPhen-2 were used to predict the structural and functional changes at the protein level., Results: A novel heterozygous mutation c.3998 G>A (p.Cys1333Tyr) was found in exon 32 in the child. The same mutation was not found among his unaffected family members and 683 healthy controls. Multiple sequence alignment showed that this novel mutation was located in a highly conserved region of the FBN1 protein across various species and may induce structural change to a functional domain., Conclusion: The novel c.3998G>A (p.Cys1333Tyr) mutation of the FBN1 gene probably predisposed the MFS in the child. Above finding has enriched the spectrum of FBN1 mutations.

Published

2018

11. [Screening and diagnostic value of the molecular markers of DNA methylation in colorectal neoplasma].

Author

Ma J, Yang Q, Deng C, Jin H, Gong W, Wang S, Chen H, and Fan Y

Subjects

Adenoma diagnosis, Biomarkers, Tumor, Cell Cycle Proteins, Colorectal Neoplasms diagnosis, Fibrillin-1 genetics, Humans, Promoter Regions, Genetic, Proteins genetics, alpha-Synuclein genetics, Adenoma genetics, Colorectal Neoplasms genetics, DNA Methylation

Abstract

Objective: To screen the molecular markers of DNA methylation with potential diagnostic value, and to explore their methylation features in Chinese colorectal neoplasma in order to find out ones with higher diagnostic value., Methods: Tissue samples of colorectal cancer and normal adjacent mucosa(>10 cm distance to tumors) from 10 colorectal cancer patients undergoing operation, and tissue samples of colorectal adenoma from 10 patients undergoing endoscopic resection in our center from June to August 2013 were collected respectively. Methylation status of 8 genes, such as SNCA, MAL, INA, SPG20, FBN1, CNRIP1, TFPI2, OSMR, was detected by BSP and qMSP to screen genes with potential diagnostic valua. ROC curve was drawn to analyze its diagnostic value., Results: BSP measurement showed that the rate of DNA methylation of SNCA, SPG20 and FBN1 was 100% in colorectal cancer and adenoma, while no methylation was found in normal adjacent mucosa. The other 5 genes expressed in different extent in cancer, adenoma and normal adjacent mucosa. Among 10 cancer tissues and normal adjacent mucosa detected by qMSP method, positive SNCA methylation was found in 5 cases and 1 case respectively; positive SPG20 in 8 cases and 1 case respectively; positive FBN1 in 7 cases and 0 cases respectively, whose differences were significant (P=0.070, P=0.003 and P=0.007). The area under curve(AUC) of SNCA, SPG20, and FBN1 methylation for diagnosing colorectal cancer was 0.890, 0.730 and 0.880 respectively., Conclusion: SNCA, SPG20 and FBN1 are potential genes with screening value for colorectal neoplasma.

Published

2015