Your search keyword '"SBF2"' showing total 11 results

1. Molecular characterization of Turkish patients with demyelinating Charcot-Marie-Tooth disease.

Author

Karakaya, Taner, Turkyilmaz, Ayberk, Sager, Gunes, Inan, Rahsan, Yarali, Oguzhan, Cebi, Alper Han, and Akin, Yasemin

Subjects

CHARCOT-Marie-Tooth disease, DEMYELINATION, TURKS, GENETIC variation, GENE therapy, MYELIN sheath diseases

Abstract

Charcot-Marie-Tooth (CMT) disease represents a distinct subgroup of inherited peripheral neuropathies with a significant prevalence throughout the world and manifests both phenotypic and genetic heterogeneity. Electrophysiological studies subclassify CMT mainly as demyelinating or axonal types. In this study, we investigated the molecular characteristics of a Turkish cohort of 23 probands out of 34 symptomatic demyelinating CMT individuals from January 2019 to December 2021. In order to identify the underlying genetic cause, we applied a rational algorithm: PMP22 gene was initially analyzed for duplication, if PMP22-duplication testing was negative, other most causative genes (GJB1, MPZ) and PMP22 were then sequenced and if no variant was detected at aforementioned tests, whole exome sequencing (WES) test was finally performed. A total of 17 patients (≅ 74%; n = 23) were found to harbor a disease-causing variant in demyelinating CMT-related genes and among the variants, PMP22-duplication was the most frequent (≅ 41%). CMT1, CMTX, and CMT4 subtypes were manifested in ten, five, and two individuals respectively. GJB1 and SBF2 genes were the only detected genes associated with the CMTs other than CMT1. We also reported totally five novel variants: c.379A > C (p.Ile127Leu) and c.548G > T (p.Arg183Leu) variants in GJB1, c.988G > T (p.Glu330Ter) variant in NEFL, c.765_770delCCCTAT (p.Pro256_Ile257del) and c.2552A > C (p.His851Pro) variants in SBF2. As the understanding of pathophysiology and molecular mechanisms of CMT continues to evolve rapidly, many therapeutic strategy options including promising small-molecular compounds, gene replacement therapy, or disease-modifying therapies will soon be implemented in the clinical setting. [ABSTRACT FROM AUTHOR]

Published

2022

2. Clinical and genetic investigation in Chinese patients with demyelinating Charcot‐Marie‐Tooth disease.

Author

He, Jin, Guo, Lingling, Xu, Guorong, Xu, Liuqing, Lin, Shan, Chen, Wanjin, and Wang, Ning

Subjects

*CHINESE people, *CHARCOT-Marie-Tooth disease, *LONGITUDINAL method, *DEMYELINATION, *GENETIC mutation, *NEUROGLIA, *POLYMERASE chain reaction, *PHENOTYPES, *SEQUENCE analysis, *SYMPTOMS, *GENETICS, *DIAGNOSIS

Abstract

Demyelinating Charcot‐Marie‐Tooth disease (CMT) is the most common subtype of CMT. It is caused mainly by 17p11.2 heterozygous duplication, but also by mutations in more than 20 genes which affect development and function of Schwann cells. To investigate the profile of genes mutated and clinical features in demyelinating CMT of Chinese descent, we collected a cohort of 44 demyelinating CMT patients and screened them using multiplex ligation‐dependent probe amplification (MLPA) and targeted next‐generation sequencing (NGS) technology. The MLPA technology revealed that 77.3% demyelinating CMT patients harbored 17p11.2 heterozygous duplication and 6.8% patients harbored heterozygous deletion of exon 6 of MPZ gene, that was further confirmed a novel c.674_675insA mutation in MPZ gene. In the patients with 17p12 heterozygous duplication, 3 sets of independent families were discordant for the CMT phenotype within the same family. The targeted NGS technology revealed that 6 candidate mutations including 1 previously reported mutation (GDAP1: c.571C>T) and 5 novel mutations (SBF2: c.415T>C, c.619G>T, c.1258A>G; GDAP1: c.589delC; PMP22: c.318delT) were found. In conclusion, combined MLPA technique with targeted NGS, the demyelinating CMT genetic diagnostic success rate was increased. [ABSTRACT FROM AUTHOR]

Published

2018

3. Novel SBF2 mutations and clinical spectrum of Charcot‐Marie‐Tooth neuropathy type 4B2.

Author

Laššuthová, P., Vill, K., Erdem‐Ozdamar, S., Schröder, J.M., Topaloglu, H., Horvath, R., Müller‐Felber, W., Bansagi, B., Schlotter‐Weigel, B., Gläser, D., Neupauerová, J., Sedláčková, L., Staněk, D., Mazanec, R., Weis, J., Seeman, P., and Senderek, J.

Subjects

*CHARCOT-Marie-Tooth disease, *GENETIC mutation, *GLAUCOMA, *ELECTROPHYSIOLOGY, *DEMYELINATION

Abstract

Biallelic SBF2 mutations cause Charcot‐Marie‐Tooth disease type 4B2 (CMT4B2), a sensorimotor neuropathy with autosomal recessive inheritance and association with glaucoma. Since the discovery of the gene mutation, only few additional patients have been reported. We identified seven CMT4B2 families with nine different SBF2 mutations. Revisiting genetic and clinical data from our cohort and the literature, SBF2 variants were private mutations, including exon‐deletion and de novo variants. The neuropathy typically started in the first decade after normal early motor development, was predominantly motor and had a rather moderate course. Electrophysiology and nerve biopsies indicated demyelination and excess myelin outfoldings constituted a characteristic feature. While neuropathy was >90% penetrant at age 10 years, glaucoma was absent in ~40% of cases but sometimes developed with age. Consequently, SBF2 mutation analysis should not be restricted to individuals with coincident neuropathy and glaucoma, and CMT4B2 patients without glaucoma should be followed for increased intraocular pressure. The presence of exon‐deletion and de novo mutations demands comprehensive mutation scanning and family studies to ensure appropriate diagnostic approaches and genetic counseling. [ABSTRACT FROM AUTHOR]

Published

2018

4. Identification of A Novel SBF2 Frameshift Mutation in Charcot–Marie–Tooth Disease Type 4B2 Using Whole-exome Sequencing

Author

Meiyan Chen, Jing Wu, Ning Liang, Lihui Tang, Yanhua Chen, Huishuang Chen, Wei Wei, Tianying Wei, Hui Huang, Xin Yi, and Ming Qi

Subjects

Whole-exome sequencing, Charcot–Marie–Tooth disease, Early-onset glaucoma, SBF2, Biology (General), QH301-705.5, Computer applications to medicine. Medical informatics, R858-859.7

Abstract

Charcot–Marie–Tooth disease type 4B2 with early-onset glaucoma (CMT4B2, OMIM 604563) is a genetically-heterogeneous childhood-onset neuromuscular disorder. Here, we report the case of a 15-year-old male adolescent with lower extremity weakness, gait abnormalities, foot deformities and early-onset glaucoma. Since clinical diagnosis alone was insufficient for providing pathogenetic evidence to indicate that the condition belonged to a consanguineous family, we applied whole-exome sequencing to samples from the patient, his parents and his younger brother, assuming that the patient’s condition is transmitted in an autosomal recessive pattern. A frame-shift mutation, c.4571delG (P.Gly1524Glufs∗42), was revealed in the CMT4B2-related gene SBF2 (also known as MTMR13, MIM 607697), and this mutation was found to be homozygous in the proband and heterozygous in his parents and younger brother. Together with the results of clinical diagnosis, this case was diagnosed as CMT4B2. Our finding further demonstrates the use of whole-exome sequencing in the diagnosis and treatment of rare diseases.

Published

2014

5. SBF1 mutations associated with autosomal recessive axonal neuropathy with cranial nerve involvement.

Author

Manole, Andreea, Horga, Alejandro, Gamez, Josep, Raguer, Nuria, Salvado, Maria, San Millán, Beatriz, Navarro, Carmen, Pittmann, Alan, Reilly, Mary, and Houlden, Henry

Abstract

Biallelic mutations in the SBF1 gene have been identified in one family with demyelinating Charcot-Marie-Tooth disease (CMT4B3) and two families with axonal neuropathy and additional neurological and skeletal features. Here we describe novel sequence variants in SBF1 (c.1168C>G and c.2209_2210del) as the potential causative mutations in two siblings with severe axonal neuropathy, hearing loss, facial weakness and bulbar features. Pathogenicity of these variants is supported by co-segregation and in silico analyses and evolutionary conservation. Our findings suggest that SBF1 mutations may cause a syndromic form of autosomal recessive axonal neuropathy (AR-CMT2) in addition to CMT4B3. [ABSTRACT FROM AUTHOR]

Published

2017

6. Identification of a novel SBF2 missense mutation associated with a rare case of thrombocytopenia using whole-exome sequencing.

Author

Abuzenadah, Adel M., Zaher, Galila F., Dallol, Ashraf, Damanhouri, Ghazi A., Chaudhary, Adeel G., Al-Sayes, Faten, Gari, Mamdooh A., AlZahrani, Mofareh, Hindawi, Salwa, and Al-Qahtani, Mohammed H.

Abstract

We describe in this report a case of a 6-years-old female who presented at the age of 1 month with a mucocutaneous bleeding and suspected thrombocytopenia. The patient’s condition was refractory to the known idiopathic thrombocytopenic purpura treatments and congenital form of Thrombocytopenia was suspected following the delivery of a male sibling with the same phenotype. The patient also manifested fair colored hair and skin relative to her family however she did not have any detectable neurologic or other immunologic abnormalities. In order to further understand this condition, we have used whole-exome sequencing of the patient’s DNA as well as her father’s with the assumption that her condition is transmitted in an autosomal recessive manner. We have identified a missense change c.659C>G (p.Thr220Arg) in the SBF2 (also known as MTMR13) gene that causes a mutation in the DENN domain of the protein. This mutation was validated by traditional Sanger sequencing and analyzed in the remaining family members were it was found to segregate in the homozygous state in the affected siblings and in the heterozygous state in both parents. This novel mutation in the DENN domain of SBF2 maybe interfering with its putative association with the Rab family of small GTPases which are important mediators of vesicle transport and membrane trafficking. In conclusion, we have identified a novel mutation that is associated with severe thrombocytopenia. The fact that this mutation is found in SBF2 gene may indicate that the underlying cause of thrombocytopenia in our patient is either a new variant form of Griscelli syndrome (through the Rab GTPases action) or a variant Charcot–Marie–Tooth type 4 disease as SBF2 truncating mutations were previously identified in sufferers of this disease. This finding will help to accurately diagnose and classify similar cases of congenital thrombocytopenia and provide further proof to the power of whole-exome sequencing in personalizing patients management from the point of diagnosis to treatment and followup. [ABSTRACT FROM AUTHOR]

Published

2013

7. Charcot-Marie-Tooth gene, SBF2, associated with taxane-induced peripheral neuropathy in African Americans

Author

Tatiana Foroud, George W. Sledge, Kathy D. Miller, Bryan P. Schneider, Gloria Xue, Guanglong Jiang, Dongbing Lai, Laura Gardner, Milan Radovich, Anne O'Neill, Fei Shen, Lang Li, and Joseph A. Sparano

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, peripheral neuropathy, Paclitaxel, Breast Neoplasms, Disease, Polymorphism, Single Nucleotide, whole exome sequencing, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Gene Frequency, Risk Factors, Internal medicine, Exome Sequencing, medicine, Humans, Genetic Predisposition to Disease, African American, Gene, Exome sequencing, Genetics, Taxane, business.industry, Cancer, Peripheral Nervous System Diseases, medicine.disease, Protein Tyrosine Phosphatases, Non-Receptor, Antineoplastic Agents, Phytogenic, Minor allele frequency, Black or African American, 030104 developmental biology, Peripheral neuropathy, Phenotype, Chemotherapy, Adjuvant, 030220 oncology & carcinogenesis, Female, business, SBF2, Research Paper

Abstract

// Bryan P. Schneider 1,* , Dongbing Lai 1,* , Fei Shen 1,* , Guanglong Jiang 1 , Milan Radovich 1 , Lang Li 1 , Laura Gardner 1 , Kathy D. Miller 1 , Anne O’Neill 2 , Joseph A. Sparano 3 , Gloria Xue 1 , Tatiana Foroud 1,** and George W. Sledge Jr. 4,** 1 Indiana University School of Medicine, Indianapolis, Indiana, USA 2 Dana Farber Cancer Institute, ECOG-ACRIN Biostatistics Center, Boston, Massachusetts, USA 3 Albert Einstein University, Montefiore Medical Center, Bronx, New York, USA 4 Stanford University School of Medicine, Stanford, California, USA * These authors have contributed equally to this work ** These authors have contributed equally to this work Correspondence to: Bryan P. Schneider, email: // Keywords : whole exome sequencing, African American, paclitaxel, peripheral neuropathy, SBF2 Received : August 29, 2016 Accepted : September 18, 2016 Published : October 09, 2016 Abstract Purpose: Taxane-induced peripheral neuropathy (TIPN) is one of the most important survivorship issues for cancer patients. African Americans (AA) have previously been shown to have an increased risk for this toxicity. Germline predictive biomarkers were evaluated to help identify a priori which patients might be at extraordinarily high risk for this toxicity. Experimental design: Whole exome sequencing was performed using germline DNA from 213 AA patients who received a standard dose and schedule of paclitaxel in the adjuvant, randomized phase III breast cancer trial, E5103. Cases were defined as those with either grade 3-4 (n=64) or grade 2-4 (n=151) TIPN and were compared to controls (n=62) that were not reported to have experienced TIPN. We retained for analysis rare variants with a minor allele frequency

Published

2016

8. Identification of a novel SBF2 frameshift mutation in charcot-marie-tooth disease type 4B2 using whole-exome sequencing

Author

Ming Qi, Wei Wei, Lihui Tang, Hui Huang, Yanhua Chen, Ning Liang, Meiyan Chen, Jing Wu, Xin Yi, Tianying Wei, and Huishuang Chen

Subjects

Proband, Male, Pediatrics, medicine.medical_specialty, Heterozygote, Adolescent, DNA Mutational Analysis, Glaucoma, Disease, Biology, Charcot–Marie–Tooth disease, Biochemistry, Frameshift mutation, Charcot-Marie-Tooth Disease, Genetics, medicine, Humans, Exome, Frameshift Mutation, lcsh:QH301-705.5, Molecular Biology, Exome sequencing, Original Research, High-Throughput Nucleotide Sequencing, Early-onset glaucoma, Heterozygote advantage, medicine.disease, Protein Tyrosine Phosphatases, Non-Receptor, Pedigree, Computational Mathematics, lcsh:Biology (General), Child, Preschool, Whole-exome sequencing, Mutation (genetic algorithm), Female, SBF2

Abstract

Charcot–Marie–Tooth disease type 4B2 with early-onset glaucoma (CMT4B2, OMIM 604563) is a genetically-heterogeneous childhood-onset neuromuscular disorder. Here, we report the case of a 15-year-old male adolescent with lower extremity weakness, gait abnormalities, foot deformities and early-onset glaucoma. Since clinical diagnosis alone was insufficient for providing pathogenetic evidence to indicate that the condition belonged to a consanguineous family, we applied whole-exome sequencing to samples from the patient, his parents and his younger brother, assuming that the patient’s condition is transmitted in an autosomal recessive pattern. A frame-shift mutation, c.4571delG (P.Gly1524Glufs∗42), was revealed in the CMT4B2-related gene SBF2 (also known as MTMR13, MIM 607697), and this mutation was found to be homozygous in the proband and heterozygous in his parents and younger brother. Together with the results of clinical diagnosis, this case was diagnosed as CMT4B2. Our finding further demonstrates the use of whole-exome sequencing in the diagnosis and treatment of rare diseases.

Published

2014

9. Charcot-Marie-Tooth gene, SBF2, associated with taxane-induced peripheral neuropathy in African Americans.

Author

Schneider BP, Lai D, Shen F, Jiang G, Radovich M, Li L, Gardner L, Miller KD, O'Neill A, Sparano JA, Xue G, Foroud T, and Sledge GW Jr

Subjects

Breast Neoplasms ethnology, Chemotherapy, Adjuvant, Female, Gene Frequency, Genetic Predisposition to Disease, Humans, Peripheral Nervous System Diseases diagnosis, Peripheral Nervous System Diseases ethnology, Phenotype, Risk Factors, Exome Sequencing, Black or African American genetics, Antineoplastic Agents, Phytogenic adverse effects, Breast Neoplasms drug therapy, Paclitaxel adverse effects, Peripheral Nervous System Diseases chemically induced, Peripheral Nervous System Diseases genetics, Polymorphism, Single Nucleotide, Protein Tyrosine Phosphatases, Non-Receptor genetics

Abstract

Purpose: Taxane-induced peripheral neuropathy (TIPN) is one of the most important survivorship issues for cancer patients. African Americans (AA) have previously been shown to have an increased risk for this toxicity. Germline predictive biomarkers were evaluated to help identify a priori which patients might be at extraordinarily high risk for this toxicity., Experimental Design: Whole exome sequencing was performed using germline DNA from 213 AA patients who received a standard dose and schedule of paclitaxel in the adjuvant, randomized phase III breast cancer trial, E5103. Cases were defined as those with either grade 3-4 (n=64) or grade 2-4 (n=151) TIPN and were compared to controls (n=62) that were not reported to have experienced TIPN. We retained for analysis rare variants with a minor allele frequency <3% and which were predicted to be deleterious by protein prediction programs. A gene-based, case-control analysis using SKAT was performed to identify genes that harbored an imbalance of deleterious variants associated with increased risk of TIPN., Results: Five genes had a p-value < 10-4 for grade 3-4 TIPN analysis and three genes had a p-value < 10-4 for the grade 2-4 TIPN analysis. For the grade 3-4 TIPN analysis, SET binding factor 2 (SBF2) was significantly associated with TIPN (p-value=4.35 x10-6). Five variants were predicted to be deleterious in SBF2. Inherited mutations in SBF2 have previously been associated with autosomal recessive, Type 4B2 Charcot-Marie-Tooth (CMT) disease., Conclusion: Rare variants in SBF2, a CMT gene, predict an increased risk of TIPN in AA patients receiving paclitaxel.

Published

2016

10. Identification of a novel SBF2 frameshift mutation in charcot-marie-tooth disease type 4B2 using whole-exome sequencing.

Author

Chen M, Wu J, Liang N, Tang L, Chen Y, Chen H, Wei W, Wei T, Huang H, Yi X, and Qi M

Subjects

Adolescent, Child, Preschool, Female, Glaucoma genetics, Heterozygote, High-Throughput Nucleotide Sequencing, Humans, Male, Pedigree, Charcot-Marie-Tooth Disease genetics, DNA Mutational Analysis methods, Exome genetics, Frameshift Mutation genetics, Protein Tyrosine Phosphatases, Non-Receptor genetics

Abstract

Charcot-Marie-Tooth disease type 4B2 with early-onset glaucoma (CMT4B2, OMIM 604563) is a genetically-heterogeneous childhood-onset neuromuscular disorder. Here, we report the case of a 15-year-old male adolescent with lower extremity weakness, gait abnormalities, foot deformities and early-onset glaucoma. Since clinical diagnosis alone was insufficient for providing pathogenetic evidence to indicate that the condition belonged to a consanguineous family, we applied whole-exome sequencing to samples from the patient, his parents and his younger brother, assuming that the patient's condition is transmitted in an autosomal recessive pattern. A frame-shift mutation, c.4571delG (P.Gly1524Glufs∗42), was revealed in the CMT4B2-related gene SBF2 (also known as MTMR13, MIM 607697), and this mutation was found to be homozygous in the proband and heterozygous in his parents and younger brother. Together with the results of clinical diagnosis, this case was diagnosed as CMT4B2. Our finding further demonstrates the use of whole-exome sequencing in the diagnosis and treatment of rare diseases., (Copyright © 2014. Production and hosting by Elsevier Ltd.)

Published

2014

11. Charcot-Marie-Tooth Hereditary Neuropathy Overview

Author

Bird TD, Adam MP, Everman DB, Mirzaa GM, Pagon RA, Wallace SE, Bean LJH, Gripp KW, and Amemiya A

Abstract

Unlabelled: The purpose of this overview is to increase the awareness of clinicians regarding Charcot-Marie-Tooth (CMT) hereditary neuropathy, its causes, and its management. The following are the goals of this overview., Goal 1: Describe the clinical characteristics of CMT hereditary neuropathy., Goal 2: Review the causes of CMT hereditary neuropathy., Goal 3: Provide an evaluation strategy to identify the cause of CMT hereditary neuropathy in a proband (when possible)., Goal 4: Inform genetic counseling of family members of an individual with CMT hereditary neuropathy., Goal 5: Review management of CMT hereditary neuropathy., (Copyright © 1993-2022, University of Washington, Seattle. GeneReviews is a registered trademark of the University of Washington, Seattle. All rights reserved.)

Published

1993