Mutation Analysis of MYORG in a Chinese Cohort With Primary Familial Brain Calcification
Primary familial brain calcification (PFBC) is a progressive neurological disorder manifesting as bilateral brain calcifications in CT scan with symptoms as parkinsonism, dystonia, ataxia, psychiatric symptoms, etc. Recently, pathogenic variants in MYORG have been linked to autosomal recessive PFBC....
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| Published in | Frontiers in genetics Vol. 12; p. 732389 |
|---|---|
| Main Authors | , , , , , , , , |
| Format | Journal Article |
| Language | English |
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Frontiers Media S.A
18.10.2021
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| ISSN | 1664-8021 1664-8021 |
| DOI | 10.3389/fgene.2021.732389 |
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| Abstract | Primary familial brain calcification (PFBC) is a progressive neurological disorder manifesting as bilateral brain calcifications in CT scan with symptoms as parkinsonism, dystonia, ataxia, psychiatric symptoms, etc. Recently, pathogenic variants in
MYORG
have been linked to autosomal recessive PFBC. This study aims to elucidate the mutational and clinical spectrum of
MYORG
mutations in a large cohort of Chinese PFBC patients with possible autosomal recessive or absent family history. Mutational analyses of
MYORG
were performed by Sanger sequencing in a cohort of 245 PFBC patients including 21 subjects from 10 families compatible with a possibly autosomal-recessive trait and 224 apparently sporadic cases. In-depth phenotyping and neuroimaging features were investigated in all patients with novel
MYORG
variants. Two nonsense variants (c.442C > T, p. Q148*; c.972C > A, p. Y324*) and two missense variants (c.1969G>C, p. G657R; c.2033C > G, p. P678R) of
MYORG
were identified in four sporadic PFBC patients, respectively. These four novel variants were absent in gnomAD, and their amino acid were highly conserved, suggesting these variants have a pathogenic impact. Patients with
MYORG
variants tend to display a homogeneous clinical spectrum, showing extensive brain calcification and parkinsonism, dysarthria, ataxia, or vertigo. Our findings supported the pathogenic role of
MYORG
variants in PFBC and identified two pathogenic variants (c.442C > T, c.972C > A), one likely pathogenic variant (c.2033C > G), and one variant of uncertain significance (c.1969G>C), further expanding the genetic and phenotypic spectrum of PFBC-
MYORG
. |
|---|---|
| AbstractList | Primary familial brain calcification (PFBC) is a progressive neurological disorder manifesting as bilateral brain calcifications in CT scan with symptoms as parkinsonism, dystonia, ataxia, psychiatric symptoms, etc. Recently, pathogenic variants in MYORG have been linked to autosomal recessive PFBC. This study aims to elucidate the mutational and clinical spectrum of MYORG mutations in a large cohort of Chinese PFBC patients with possible autosomal recessive or absent family history. Mutational analyses of MYORG were performed by Sanger sequencing in a cohort of 245 PFBC patients including 21 subjects from 10 families compatible with a possibly autosomal-recessive trait and 224 apparently sporadic cases. In-depth phenotyping and neuroimaging features were investigated in all patients with novel MYORG variants. Two nonsense variants (c.442C > T, p. Q148*; c.972C > A, p. Y324*) and two missense variants (c.1969G>C, p. G657R; c.2033C > G, p. P678R) of MYORG were identified in four sporadic PFBC patients, respectively. These four novel variants were absent in gnomAD, and their amino acid were highly conserved, suggesting these variants have a pathogenic impact. Patients with MYORG variants tend to display a homogeneous clinical spectrum, showing extensive brain calcification and parkinsonism, dysarthria, ataxia, or vertigo. Our findings supported the pathogenic role of MYORG variants in PFBC and identified two pathogenic variants (c.442C > T, c.972C > A), one likely pathogenic variant (c.2033C > G), and one variant of uncertain significance (c.1969G>C), further expanding the genetic and phenotypic spectrum of PFBC-MYORG. Primary familial brain calcification (PFBC) is a progressive neurological disorder manifesting as bilateral brain calcifications in CT scan with symptoms as parkinsonism, dystonia, ataxia, psychiatric symptoms, etc. Recently, pathogenic variants in MYORG have been linked to autosomal recessive PFBC. This study aims to elucidate the mutational and clinical spectrum of MYORG mutations in a large cohort of Chinese PFBC patients with possible autosomal recessive or absent family history. Mutational analyses of MYORG were performed by Sanger sequencing in a cohort of 245 PFBC patients including 21 subjects from 10 families compatible with a possibly autosomal-recessive trait and 224 apparently sporadic cases. In-depth phenotyping and neuroimaging features were investigated in all patients with novel MYORG variants. Two nonsense variants (c.442C > T, p. Q148*; c.972C > A, p. Y324*) and two missense variants (c.1969G>C, p. G657R; c.2033C > G, p. P678R) of MYORG were identified in four sporadic PFBC patients, respectively. These four novel variants were absent in gnomAD, and their amino acid were highly conserved, suggesting these variants have a pathogenic impact. Patients with MYORG variants tend to display a homogeneous clinical spectrum, showing extensive brain calcification and parkinsonism, dysarthria, ataxia, or vertigo. Our findings supported the pathogenic role of MYORG variants in PFBC and identified two pathogenic variants (c.442C > T, c.972C > A), one likely pathogenic variant (c.2033C > G), and one variant of uncertain significance (c.1969G>C), further expanding the genetic and phenotypic spectrum of PFBC- MYORG . Primary familial brain calcification (PFBC) is a progressive neurological disorder manifesting as bilateral brain calcifications in CT scan with symptoms as parkinsonism, dystonia, ataxia, psychiatric symptoms, etc. Recently, pathogenic variants in MYORG have been linked to autosomal recessive PFBC. This study aims to elucidate the mutational and clinical spectrum of MYORG mutations in a large cohort of Chinese PFBC patients with possible autosomal recessive or absent family history. Mutational analyses of MYORG were performed by Sanger sequencing in a cohort of 245 PFBC patients including 21 subjects from 10 families compatible with a possibly autosomal-recessive trait and 224 apparently sporadic cases. In-depth phenotyping and neuroimaging features were investigated in all patients with novel MYORG variants. Two nonsense variants (c.442C > T, p. Q148*; c.972C > A, p. Y324*) and two missense variants (c.1969G>C, p. G657R; c.2033C > G, p. P678R) of MYORG were identified in four sporadic PFBC patients, respectively. These four novel variants were absent in gnomAD, and their amino acid were highly conserved, suggesting these variants have a pathogenic impact. Patients with MYORG variants tend to display a homogeneous clinical spectrum, showing extensive brain calcification and parkinsonism, dysarthria, ataxia, or vertigo. Our findings supported the pathogenic role of MYORG variants in PFBC and identified two pathogenic variants (c.442C > T, c.972C > A), one likely pathogenic variant (c.2033C > G), and one variant of uncertain significance (c.1969G>C), further expanding the genetic and phenotypic spectrum of PFBC-MYORG.Primary familial brain calcification (PFBC) is a progressive neurological disorder manifesting as bilateral brain calcifications in CT scan with symptoms as parkinsonism, dystonia, ataxia, psychiatric symptoms, etc. Recently, pathogenic variants in MYORG have been linked to autosomal recessive PFBC. This study aims to elucidate the mutational and clinical spectrum of MYORG mutations in a large cohort of Chinese PFBC patients with possible autosomal recessive or absent family history. Mutational analyses of MYORG were performed by Sanger sequencing in a cohort of 245 PFBC patients including 21 subjects from 10 families compatible with a possibly autosomal-recessive trait and 224 apparently sporadic cases. In-depth phenotyping and neuroimaging features were investigated in all patients with novel MYORG variants. Two nonsense variants (c.442C > T, p. Q148*; c.972C > A, p. Y324*) and two missense variants (c.1969G>C, p. G657R; c.2033C > G, p. P678R) of MYORG were identified in four sporadic PFBC patients, respectively. These four novel variants were absent in gnomAD, and their amino acid were highly conserved, suggesting these variants have a pathogenic impact. Patients with MYORG variants tend to display a homogeneous clinical spectrum, showing extensive brain calcification and parkinsonism, dysarthria, ataxia, or vertigo. Our findings supported the pathogenic role of MYORG variants in PFBC and identified two pathogenic variants (c.442C > T, c.972C > A), one likely pathogenic variant (c.2033C > G), and one variant of uncertain significance (c.1969G>C), further expanding the genetic and phenotypic spectrum of PFBC-MYORG. |
| Author | Yao, Xiang-Ping Su, Hui-Zhen Guo, Xin-Xin Li, Yun-Lu Chen, Wan-Jin Zhao, Miao Lai, Lu-Lu Lin, Bi-Wei Zeng, Yi-Heng |
| AuthorAffiliation | Department of Neurology and Institute of Neurology of First Affiliated Hospital, Institute of Neuroscience, and Fujian Key Laboratory of Molecular Neurology, Fujian Medical University, Fuzhou , China |
| AuthorAffiliation_xml | – name: Department of Neurology and Institute of Neurology of First Affiliated Hospital, Institute of Neuroscience, and Fujian Key Laboratory of Molecular Neurology, Fujian Medical University, Fuzhou , China |
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| CitedBy_id | crossref_primary_10_1002_mgg3_2276 crossref_primary_10_3390_ijms241310886 crossref_primary_10_1016_j_parkreldis_2025_107290 crossref_primary_10_1007_s12264_022_00980_0 crossref_primary_10_3389_fneur_2023_1110227 crossref_primary_10_1016_j_gene_2023_147213 |
| Cites_doi | 10.1002/ajmg.b.32605 10.1038/ng.3289 10.1038/ng.2723 10.1007/s10072-015-2110-8 10.1212/wnl.0b013e31827ccf34 10.1093/brain/awz392 10.1212/nxg.0000000000000399 10.1038/ng.1077 10.1002/mds.27973 10.1016/j.neuron.2018.05.037 10.1097/wco.0000000000000712 10.1016/j.parkreldis.2004.12.001 10.1038/s10038-020-0779-x 10.1093/brain/awt255 10.1007/s10048-019-00571-8 10.1093/brain/awz095 10.1038/gim.2015.30 10.1016/j.parkreldis.2019.09.021 10.1007/s11910-019-0986-z 10.1074/jbc.m109.034041 10.1093/brain/awy343 10.1002/humu.23703 10.1002/mds.27582 |
| ContentType | Journal Article |
| Copyright | Copyright © 2021 Zeng, Lin, Su, Guo, Li, Lai, Chen, Zhao and Yao. Copyright © 2021 Zeng, Lin, Su, Guo, Li, Lai, Chen, Zhao and Yao. 2021 Zeng, Lin, Su, Guo, Li, Lai, Chen, Zhao and Yao |
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| References | Richards (B18) 2015; 17 Chen (B4) 2020; 35 Chen (B5) 2019; 34 Keller (B10) 2013; 45 Yao (B23) 2018; 98 Grangeon (B8) 2019; 142 Nicolas (B16) 2013; 80 Westenberger (B22) 2019; 32 Nicolas (B15) 2013; 136 Forouhideh (B7) 2019; 142 Taglia (B19) 2015; 36 Kume (B11) 2020; 65 Legati (B12) 2015; 47 Wang (B21) 2012; 44 Bauer (B1) 2019; 19 Cen (B2) 2020; 143 Datta (B6) 2009; 284 Manyam (B13) 2005; 11 Guo (B9) 2019; 40 Nicolas (B14) 2018; 177 Chelban (B3) 2020; 6 Ramos (B17) 2019; 20 Taglia (B20) 2019; 67 |
| References_xml | – volume: 177 start-page: 68 year: 2018 ident: B14 article-title: Estimation of Minimal Disease Prevalence from Population Genomic Data: Application to Primary Familial Brain Calcification publication-title: Am. J. Med. Genet. doi: 10.1002/ajmg.b.32605 – volume: 47 start-page: 579 year: 2015 ident: B12 article-title: Mutations in XPR1 Cause Primary Familial Brain Calcification Associated with Altered Phosphate export publication-title: Nat. Genet. doi: 10.1038/ng.3289 – volume: 45 start-page: 1077 year: 2013 ident: B10 article-title: Mutations in the Gene Encoding PDGF-B Cause Brain Calcifications in Humans and Mice publication-title: Nat. Genet. doi: 10.1038/ng.2723 – volume: 36 start-page: 787 year: 2015 ident: B19 article-title: Primary Familial Brain Calcification: Update on Molecular Genetics publication-title: Neurol. Sci. doi: 10.1007/s10072-015-2110-8 – volume: 80 start-page: 181 year: 2013 ident: B16 article-title: Mutation of the PDGFRB Gene as a Cause of Idiopathic Basal Ganglia Calcification publication-title: Neurology doi: 10.1212/wnl.0b013e31827ccf34 – volume: 143 start-page: 491 year: 2020 ident: B2 article-title: Biallelic Loss-Of-Function Mutations in JAM2 Cause Primary Familial Brain Calcification publication-title: Brain doi: 10.1093/brain/awz392 – volume: 6 start-page: e399 year: 2020 ident: B3 article-title: MYORG-Related Disease Is Associated with Central Pontine Calcifications and Atypical Parkinsonism publication-title: Neurol. Genet. doi: 10.1212/nxg.0000000000000399 – volume: 44 start-page: 254 year: 2012 ident: B21 article-title: Mutations in SLC20A2 Link Familial Idiopathic Basal Ganglia Calcification with Phosphate Homeostasis publication-title: Nat. Genet. doi: 10.1038/ng.1077 – volume: 35 start-page: 679 year: 2020 ident: B4 article-title: MYORG Mutation Heterozygosity Is Associated with Brain Calcification publication-title: Mov Disord. doi: 10.1002/mds.27973 – volume: 98 start-page: 1116 year: 2018 ident: B23 article-title: Biallelic Mutations in MYORG Cause Autosomal Recessive Primary Familial Brain Calcification publication-title: Neuron doi: 10.1016/j.neuron.2018.05.037 – volume: 32 start-page: 571 year: 2019 ident: B22 article-title: Primary Familial Brain Calcifications: Genetic and Clinical Update publication-title: Curr. Opin. Neurol. doi: 10.1097/wco.0000000000000712 – volume: 11 start-page: 73 year: 2005 ident: B13 article-title: What Is and what Is Not 'Fahr's Disease' publication-title: Parkinsonism Relat. Disord. doi: 10.1016/j.parkreldis.2004.12.001 – volume: 65 start-page: 917 year: 2020 ident: B11 article-title: The First Japanese Case of Primary Familial Brain Calcification Caused by an MYORG Variant publication-title: J. Hum. Genet. doi: 10.1038/s10038-020-0779-x – volume: 136 start-page: 3395 year: 2013 ident: B15 article-title: Phenotypic Spectrum of Probable and Genetically-Confirmed Idiopathic Basal Ganglia Calcification publication-title: Brain doi: 10.1093/brain/awt255 – volume: 20 start-page: 99 year: 2019 ident: B17 article-title: Primary Familial Brain Calcification Caused by a Novel Homozygous MYORG Mutation in a Consanguineous Italian Family publication-title: Neurogenetics doi: 10.1007/s10048-019-00571-8 – volume: 142 start-page: 1573 year: 2019 ident: B8 article-title: Biallelic MYORG Mutation Carriers Exhibit Primary Brain Calcification with a Distinct Phenotype publication-title: Brain doi: 10.1093/brain/awz095 – volume: 17 start-page: 405 year: 2015 ident: B18 article-title: Standards and Guidelines for the Interpretation of Sequence Variants: a Joint Consensus Recommendation of the American College of Medical Genetics and Genomics and the Association for Molecular Pathology publication-title: Genet. Med. doi: 10.1038/gim.2015.30 – volume: 67 start-page: 24 year: 2019 ident: B20 article-title: Primary Familial Brain Calcification Caused by MYORG Mutations in an Italian Family publication-title: Parkinsonism Relat. Disord. doi: 10.1016/j.parkreldis.2019.09.021 – volume: 19 start-page: 70 year: 2019 ident: B1 article-title: MYORG Mutations: A Major Cause of Recessive Primary Familial Brain Calcification publication-title: Curr. Neurol. Neurosci. Rep. doi: 10.1007/s11910-019-0986-z – volume: 284 start-page: 29666 year: 2009 ident: B6 article-title: NET37, a Nuclear Envelope Transmembrane Protein with Glycosidase Homology, Is Involved in Myoblast Differentiation publication-title: J. Biol. Chem. doi: 10.1074/jbc.m109.034041 – volume: 142 start-page: e4 year: 2019 ident: B7 article-title: A Biallelic Mutation linksMYORGto Autosomal-Recessive Primary Familial Brain Calcification publication-title: Brain doi: 10.1093/brain/awy343 – volume: 40 start-page: 392 year: 2019 ident: B9 article-title: Spectrum of SLC20A2 , PDGFRB , PDGFB , and XPR1 Mutations in a Large Cohort of Patients with Primary Familial Brain Calcification publication-title: Hum. Mutat. doi: 10.1002/humu.23703 – volume: 34 start-page: 291 year: 2019 ident: B5 article-title: Evaluation of MYORG Mutations as a Novel Cause of Primary Familial Brain Calcification publication-title: Mov Disord. doi: 10.1002/mds.27582 |
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| Title | Mutation Analysis of MYORG in a Chinese Cohort With Primary Familial Brain Calcification |
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