GWAS on prolonged gestation (post-term birth): analysis of successive Finnish birth cohorts.

Background Gestation is a crucial timepoint in human development. Deviation from a term gestational age correlates with both acute and long-term adverse health effects for the child. Both being born preterm and post-term, that is, having short and long gestational ages, are heritable and influenced...

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Bibliographic Details
Published in:Journal of Medical Genetics
Main Authors: Schierding, W, Antony, J, Karhunen, V, Vaarasmaki, M, Franks, S, Elliott, P, Kajantie, E, Sebert, S, Blakemore, A, Horsfield, JA, Jarvelin, MR, O'Sullivan, J, Cutfield, WS
Other Authors: Medical Research Council (MRC)
Format: Article in Journal/Newspaper
Language:unknown
Published: BMJ Publishing Group 2017
Subjects:
Science & Technology
Life Sciences & Biomedicine
Genetics & Heredity
GENOME-WIDE ASSOCIATION
INSULIN-RESISTANCE
GENETIC INFLUENCE
BORN PRETERM
RISK-FACTORS
PREGNANCY
DELIVERY
VARIANTS
FETAL
RECURRENCE
adamts13
b3galt5
gwas
post-term
prolonged gestation
06 Biological Sciences
11 Medical And Health Sciences
Northern Finland
Online Access:http://hdl.handle.net/10044/1/50802
https://doi.org/10.1136/jmedgenet-2017-104880
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Summary:Background Gestation is a crucial timepoint in human development. Deviation from a term gestational age correlates with both acute and long-term adverse health effects for the child. Both being born preterm and post-term, that is, having short and long gestational ages, are heritable and influenced by the prenatal and perinatal environment. Despite the obvious heritable component, specific genetic influences underlying differences in gestational age are poorly understood. Methods We investigated the genetic architecture of gestational age in 9141 individuals, including 1167 born post-term, across two Northern Finland cohorts born in 1966 or 1986. Results Here we identify one globally significant intronic genetic variant within the ADAMTS13 gene that is associated with prolonged gestation (p=4.85×10−8). Additional variants that reached suggestive levels of significance were identified within introns at the ARGHAP42 and TKT genes, and in the upstream (5’) intergenic regions of the B3GALT5 and SSBP2 genes. The variants near the ADAMTS13, B3GALT5, SSBP2 and TKT loci are linked to alterations in gene expression levels (cis-eQTLs). Luciferase assays confirmed the allele specific enhancer activity for the BGALT5 and TKT loci. Conclusions Our findings provide the first evidence of a specific genetic influence associated with prolonged gestation. This study forms a foundation for a better understanding of the genetic and long-term health risks faced by induced and post-term individuals. The long-term risks for induced individuals who have a previously overlooked post-term potential may be a major issue for current health providers.

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