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Targeted Sequencing of Candidate Regions Associated with Sagittal and Metopic Nonsyndromic Craniosynostosis. | LitMetric

AI Article Synopsis

  • Craniosynostosis (CS) is a significant birth defect where skull bones fuse too early; research has identified genetic associations linked to this condition.
  • A genome-wide association study (GWAS) revealed specific genetic regions associated with both sagittal non-syndromic CS (sNCS) and metopic non-syndromic CS (mNCS), leading to further sequencing of these areas in child-parent trios.
  • The study focuses on variants within these genetic regions that are predicted to impact transcription factors related to craniofacial and bone development, prioritizing those with potential detrimental effects for further investigation.

Article Abstract

Craniosynostosis (CS) is a major birth defect in which one or more skull sutures fuse prematurely. We previously performed a genome-wide association study (GWAS) for sagittal non-syndromic CS (sNCS), identifying associations downstream from on 20p12.3 and intronic to on 7p14.3; analyses of imputed variants in on 3q29 were also genome-wide significant. We followed this work with a GWAS for metopic non-syndromic NCS (mNCS), discovering a significant association intronic to on 20q13.31. In the current study, we sequenced the associated regions on 3q29, 7p14.3, and 20p12.3, including two candidate genes ( and near some of these regions in 83 sNCS child-parent trios, and sequenced regions on 7p14.3 and 20q13.2-q13.32 in 80 mNCS child-parent trios. These child-parent trios were selected from the original GWAS cohorts if the probands carried at least one copy of the top associated GWAS variant (rs1884302 C allele for sNCS; rs6127972 T allele for mNCS). Many of the variants sequenced in these targeted regions are strongly predicted to be within binding sites for transcription factors involved in craniofacial development or bone morphogenesis. Variants enriched in more than one trio and predicted to be damaging to gene function are prioritized for functional studies.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9141801PMC
http://dx.doi.org/10.3390/genes13050816DOI Listing

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