Novel MEF2C point mutations in Chinese patients with Rett (−like) syndrome or non-syndromic intellectual disability: insights into genotype-phenotype correlation

Novel MEF2C point mutations in Chinese patients with Rett (−like) syndrome or non-syndromic intellectual disability: insights into genotype-phenotype correlation

Abstract Background MEF2C (Myocyte-specific enhancer factor 2C) has been associated with neurodevelopmental disorders. This study aimed at delineating the clinical profiles of MEF2C gene mutations. Methods In total, 112 Chinese patients with intellectual disability (ID) were recruited, including 44...

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Main Authors: Jiaping Wang, Qingping Zhang, Yan Chen, Shujie Yu, Xiru Wu, Xinhua Bao, Yongxin Wen
Format: Article
Language:English
Published: BMC 2018-10-01
Series:BMC Medical Genetics
Subjects:
MEF2C
Rett (−like) syndrome
Non-syndromic intellectual disability
Genotype-phenotype correlation
Online Access:http://link.springer.com/article/10.1186/s12881-018-0699-1
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spelling doaj-21119a45ae4342078d20f37d0bfab9782021-04-02T12:29:29ZengBMCBMC Medical Genetics1471-23502018-10-011911610.1186/s12881-018-0699-1Novel MEF2C point mutations in Chinese patients with Rett (−like) syndrome or non-syndromic intellectual disability: insights into genotype-phenotype correlationJiaping Wang0Qingping Zhang1Yan Chen2Shujie Yu3Xiru Wu4Xinhua Bao5Yongxin Wen6Department of Pediatrics, Peking University First HospitalDepartment of Pediatrics, Peking University First HospitalDepartment of Pediatrics, Peking University First HospitalDepartment of neurology, Harbin children’s hospitalDepartment of Pediatrics, Peking University First HospitalDepartment of Pediatrics, Peking University First HospitalDepartment of Pediatrics, Peking University First HospitalAbstract Background MEF2C (Myocyte-specific enhancer factor 2C) has been associated with neurodevelopmental disorders. This study aimed at delineating the clinical profiles of MEF2C gene mutations. Methods In total, 112 Chinese patients with intellectual disability (ID) were recruited, including 44 patients presented with Rett syndrome (RTT) or RTT-like syndrome, and 68 patients with non-syndromic ID. Targeted next-generation sequencing (NGS) was performed. Detailed clinical information was collected. Results Five heterozygous MEF2C gene mutations were identified, of which three were novel. The MEF2C mutant rate was 4.5% (5/112) in total, and 6.8% (3/44) in the RTT (−like) cohort. All patients with MEF2C gene mutation presented with cognitive impairment, gross motor delay, speech disorder and autistic features. Four patients had epilepsy, which responded well to antiepileptic drugs. One female was diagnosed with classical RTT, two females with RTT-like syndrome, and two males with non-syndromic ID. Generally, the phenotype of two males with relatively downstream mutations (c.565C > T, p.Arg 189*; c.766C > T, p.Arg 256*) was milder than that of three females with upstream mutations (c.48C > G, p.Asn16Lys; c.334G > T, p.Glu112* and c.403-1G > T). Conclusions Our findings expanded the current understanding of the consequences of MEF2C dysfunctions, especially MEF2C point mutations. MEF2C mutations are associated with a broad clinical spectrum, ranged from classical RTT to non-syndromic ID. Through our study, it can be inferred that there is correlation between the phenotype and MEF2C-genotype, the mutation site. Overall, the MEF2C gene mutational analysis should be performed in ID cohort, especially in patients with features overlapped with RTT.http://link.springer.com/article/10.1186/s12881-018-0699-1MEF2CRett (−like) syndromeNon-syndromic intellectual disabilityGenotype-phenotype correlation
collection DOAJ
language English
format Article
sources DOAJ
author Jiaping Wang
Qingping Zhang
Yan Chen
Shujie Yu
Xiru Wu
Xinhua Bao
Yongxin Wen
spellingShingle Jiaping Wang
Qingping Zhang
Yan Chen
Shujie Yu
Xiru Wu
Xinhua Bao
Yongxin Wen
Novel MEF2C point mutations in Chinese patients with Rett (−like) syndrome or non-syndromic intellectual disability: insights into genotype-phenotype correlation
BMC Medical Genetics
MEF2C
Rett (−like) syndrome
Non-syndromic intellectual disability
Genotype-phenotype correlation
author_facet Jiaping Wang
Qingping Zhang
Yan Chen
Shujie Yu
Xiru Wu
Xinhua Bao
Yongxin Wen
author_sort Jiaping Wang
title Novel MEF2C point mutations in Chinese patients with Rett (−like) syndrome or non-syndromic intellectual disability: insights into genotype-phenotype correlation
title_short Novel MEF2C point mutations in Chinese patients with Rett (−like) syndrome or non-syndromic intellectual disability: insights into genotype-phenotype correlation
title_full Novel MEF2C point mutations in Chinese patients with Rett (−like) syndrome or non-syndromic intellectual disability: insights into genotype-phenotype correlation
title_fullStr Novel MEF2C point mutations in Chinese patients with Rett (−like) syndrome or non-syndromic intellectual disability: insights into genotype-phenotype correlation
title_full_unstemmed Novel MEF2C point mutations in Chinese patients with Rett (−like) syndrome or non-syndromic intellectual disability: insights into genotype-phenotype correlation
title_sort novel mef2c point mutations in chinese patients with rett (−like) syndrome or non-syndromic intellectual disability: insights into genotype-phenotype correlation
publisher BMC
series BMC Medical Genetics
issn 1471-2350
publishDate 2018-10-01
description Abstract Background MEF2C (Myocyte-specific enhancer factor 2C) has been associated with neurodevelopmental disorders. This study aimed at delineating the clinical profiles of MEF2C gene mutations. Methods In total, 112 Chinese patients with intellectual disability (ID) were recruited, including 44 patients presented with Rett syndrome (RTT) or RTT-like syndrome, and 68 patients with non-syndromic ID. Targeted next-generation sequencing (NGS) was performed. Detailed clinical information was collected. Results Five heterozygous MEF2C gene mutations were identified, of which three were novel. The MEF2C mutant rate was 4.5% (5/112) in total, and 6.8% (3/44) in the RTT (−like) cohort. All patients with MEF2C gene mutation presented with cognitive impairment, gross motor delay, speech disorder and autistic features. Four patients had epilepsy, which responded well to antiepileptic drugs. One female was diagnosed with classical RTT, two females with RTT-like syndrome, and two males with non-syndromic ID. Generally, the phenotype of two males with relatively downstream mutations (c.565C > T, p.Arg 189*; c.766C > T, p.Arg 256*) was milder than that of three females with upstream mutations (c.48C > G, p.Asn16Lys; c.334G > T, p.Glu112* and c.403-1G > T). Conclusions Our findings expanded the current understanding of the consequences of MEF2C dysfunctions, especially MEF2C point mutations. MEF2C mutations are associated with a broad clinical spectrum, ranged from classical RTT to non-syndromic ID. Through our study, it can be inferred that there is correlation between the phenotype and MEF2C-genotype, the mutation site. Overall, the MEF2C gene mutational analysis should be performed in ID cohort, especially in patients with features overlapped with RTT.
topic MEF2C
Rett (−like) syndrome
Non-syndromic intellectual disability
Genotype-phenotype correlation
url http://link.springer.com/article/10.1186/s12881-018-0699-1
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