De novo mutations in ARID1B associated with both syndromic and non-syndromic short stature.

BMC Genomics
Authors
Keywords
Abstract

BACKGROUND: Human height is a complex trait with a strong genetic basis. Recently, a significant association between rare copy number variations (CNVs) and short stature has been identified, and candidate genes in these rare CNVs are being explored. This study aims to evaluate the association between mutations in ARID1B gene and short stature, both the syndromic and non-syndromic form.

RESULTS: Based on a case-control study of whole genome chromosome microarray analysis (CMA), three overlapping CNVs were identified in patients with developmental disorders who exhibited short stature. ARID1B, a causal gene for Coffin Siris syndrome, is the only gene encompassed by all three CNVs. A following retrospective genotype-phenotype analysis based on a literature review confirmed that short stature is a frequent feature in those Coffin-Siris syndrome patients with ARID1B mutations. Mutation screening of ARID1B coding regions was further conducted in a cohort of 48 non-syndromic short stature patients,andfour novel missense variants including two de novo mutations were found.

CONCLUSION: These results suggest that haploinsufficient mutations of ARID1B are associated with syndromic short stature including Coffin-Siris syndrome and intellectual disability, while rare missense variants in ARID1B are associated with non-syndromic short stature. This study supports the notion that mutations in genes related to syndromic short stature may exert milder effect and contribute to short stature in the general population.

Year of Publication
2015
Journal
BMC Genomics
Volume
16
Pages
701
Date Published
2015 Sep 16
ISSN
1471-2164
URL
DOI
10.1186/s12864-015-1898-1
PubMed ID
26376624
PubMed Central ID
PMC4574214
Links
Grant list
K23 HD073351 / HD / NICHD NIH HHS / United States
5K23HD073351 / HD / NICHD NIH HHS / United States