A New Role for LOC101928437 in Non-Syndromic Intellectual Disability: Findings from a Family-Based Association Test

Non-syndromic intellectual disability (NSID) is mental retardation in persons of normal physical appearance who have no recognisable features apart from obvious deficits in intellectual functioning and adaptive ability; however, its genetic etiology of most patients has remained unknown. The main pu...

Descripción completa

Detalles Bibliográficos
Autores principales: Zhou, Shaohe, Shi, Zhangyan, Cui, Meng, Li, Junlin, Ma, Zhe, Shi, Yuanyu, Zheng, Zijian, Zhang, Fuchang, Jin, Tianbo, Geng, Tingting, Chen, Chao, Guo, Yale, Zhou, Jianping, Huang, Shaoping, Guo, Xingli, Gao, Lin, Gong, Pingyuan, Gao, Xiaocai, Zhang, Kejin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4545728/
https://www.ncbi.nlm.nih.gov/pubmed/26287547
http://dx.doi.org/10.1371/journal.pone.0135669
_version_ 1782386775080042496
author Zhou, Shaohe
Shi, Zhangyan
Cui, Meng
Li, Junlin
Ma, Zhe
Shi, Yuanyu
Zheng, Zijian
Zhang, Fuchang
Jin, Tianbo
Geng, Tingting
Chen, Chao
Guo, Yale
Zhou, Jianping
Huang, Shaoping
Guo, Xingli
Gao, Lin
Gong, Pingyuan
Gao, Xiaocai
Zhang, Kejin
author_facet Zhou, Shaohe
Shi, Zhangyan
Cui, Meng
Li, Junlin
Ma, Zhe
Shi, Yuanyu
Zheng, Zijian
Zhang, Fuchang
Jin, Tianbo
Geng, Tingting
Chen, Chao
Guo, Yale
Zhou, Jianping
Huang, Shaoping
Guo, Xingli
Gao, Lin
Gong, Pingyuan
Gao, Xiaocai
Zhang, Kejin
author_sort Zhou, Shaohe
collection PubMed
description Non-syndromic intellectual disability (NSID) is mental retardation in persons of normal physical appearance who have no recognisable features apart from obvious deficits in intellectual functioning and adaptive ability; however, its genetic etiology of most patients has remained unknown. The main purpose of this study was to fine map and identify specific causal gene(s) by genotyping a NSID family cohort using a panel of markers encompassing a target region reported in a previous work. A total of 139 families including probands, parents and relatives were included in the household survey, clinical examinations and intelligence tests, recruited from the Qinba mountain region of Shannxi province, western China. A collection of 34 tagged single nucleotide polymorphisms (tSNPs) spanning five microsatellite marker (STR) loci were genotyped using an iPLEX Gold assay. The association between tSNPs and patients was analyzed by family-based association testing (FBAT) and haplotype analysis (HBAT). Four markers (rs5974392, rs12164331, rs5929554 and rs3116911) in a block that showed strong linkage disequilibrium within the first three introns of the LOC 101928437 locus were found to be significantly associated with NSID (all P<0.01) by the FBAT method for a single marker in additive, dominant and recessive models. The results of haplotype tests of this block also revealed a significant association with NSID (all P<0.05) using 2-window and larger HBAT analyses. These results suggest that LOC 101928437 is a novel candidate gene for NSID in Han Chinese individuals of the Qinba region of China. Although the biological function of the gene has not been well studied, knowledge about this gene will provide insights that will increase our understanding of NSID development.
format Online
Article
Text
id pubmed-4545728
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-45457282015-09-01 A New Role for LOC101928437 in Non-Syndromic Intellectual Disability: Findings from a Family-Based Association Test Zhou, Shaohe Shi, Zhangyan Cui, Meng Li, Junlin Ma, Zhe Shi, Yuanyu Zheng, Zijian Zhang, Fuchang Jin, Tianbo Geng, Tingting Chen, Chao Guo, Yale Zhou, Jianping Huang, Shaoping Guo, Xingli Gao, Lin Gong, Pingyuan Gao, Xiaocai Zhang, Kejin PLoS One Research Article Non-syndromic intellectual disability (NSID) is mental retardation in persons of normal physical appearance who have no recognisable features apart from obvious deficits in intellectual functioning and adaptive ability; however, its genetic etiology of most patients has remained unknown. The main purpose of this study was to fine map and identify specific causal gene(s) by genotyping a NSID family cohort using a panel of markers encompassing a target region reported in a previous work. A total of 139 families including probands, parents and relatives were included in the household survey, clinical examinations and intelligence tests, recruited from the Qinba mountain region of Shannxi province, western China. A collection of 34 tagged single nucleotide polymorphisms (tSNPs) spanning five microsatellite marker (STR) loci were genotyped using an iPLEX Gold assay. The association between tSNPs and patients was analyzed by family-based association testing (FBAT) and haplotype analysis (HBAT). Four markers (rs5974392, rs12164331, rs5929554 and rs3116911) in a block that showed strong linkage disequilibrium within the first three introns of the LOC 101928437 locus were found to be significantly associated with NSID (all P<0.01) by the FBAT method for a single marker in additive, dominant and recessive models. The results of haplotype tests of this block also revealed a significant association with NSID (all P<0.05) using 2-window and larger HBAT analyses. These results suggest that LOC 101928437 is a novel candidate gene for NSID in Han Chinese individuals of the Qinba region of China. Although the biological function of the gene has not been well studied, knowledge about this gene will provide insights that will increase our understanding of NSID development. Public Library of Science 2015-08-19 /pmc/articles/PMC4545728/ /pubmed/26287547 http://dx.doi.org/10.1371/journal.pone.0135669 Text en © 2015 Zhou et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Zhou, Shaohe
Shi, Zhangyan
Cui, Meng
Li, Junlin
Ma, Zhe
Shi, Yuanyu
Zheng, Zijian
Zhang, Fuchang
Jin, Tianbo
Geng, Tingting
Chen, Chao
Guo, Yale
Zhou, Jianping
Huang, Shaoping
Guo, Xingli
Gao, Lin
Gong, Pingyuan
Gao, Xiaocai
Zhang, Kejin
A New Role for LOC101928437 in Non-Syndromic Intellectual Disability: Findings from a Family-Based Association Test
title A New Role for LOC101928437 in Non-Syndromic Intellectual Disability: Findings from a Family-Based Association Test
title_full A New Role for LOC101928437 in Non-Syndromic Intellectual Disability: Findings from a Family-Based Association Test
title_fullStr A New Role for LOC101928437 in Non-Syndromic Intellectual Disability: Findings from a Family-Based Association Test
title_full_unstemmed A New Role for LOC101928437 in Non-Syndromic Intellectual Disability: Findings from a Family-Based Association Test
title_short A New Role for LOC101928437 in Non-Syndromic Intellectual Disability: Findings from a Family-Based Association Test
title_sort new role for loc101928437 in non-syndromic intellectual disability: findings from a family-based association test
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4545728/
https://www.ncbi.nlm.nih.gov/pubmed/26287547
http://dx.doi.org/10.1371/journal.pone.0135669
work_keys_str_mv AT zhoushaohe anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT shizhangyan anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT cuimeng anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT lijunlin anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT mazhe anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT shiyuanyu anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT zhengzijian anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT zhangfuchang anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT jintianbo anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT gengtingting anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT chenchao anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT guoyale anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT zhoujianping anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT huangshaoping anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT guoxingli anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT gaolin anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT gongpingyuan anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT gaoxiaocai anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT zhangkejin anewroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT zhoushaohe newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT shizhangyan newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT cuimeng newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT lijunlin newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT mazhe newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT shiyuanyu newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT zhengzijian newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT zhangfuchang newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT jintianbo newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT gengtingting newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT chenchao newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT guoyale newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT zhoujianping newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT huangshaoping newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT guoxingli newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT gaolin newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT gongpingyuan newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT gaoxiaocai newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest
AT zhangkejin newroleforloc101928437innonsyndromicintellectualdisabilityfindingsfromafamilybasedassociationtest

Ejemplares similares