Haplotype-based analysis distinguishes maternal-fetal genetic contribution to pregnancy-related outcomes
Srivastava, Amit K; Juodakis, Julius; Sole-Navais, Pol; Chen, Jing; Bacelis, Jonas; Teramo, Kari; Hallman, Mikko; Njølstad, Pal R; Evans, David M; Jacobsson, Bo; Muglia, Louis J; Zhang, Ge (2025-03-10)
Public Library of Science (PLoS)
10.03.2025
Srivastava AK, Juodakis J, Sole-Navais P, Chen J, Bacelis J, Teramo K, et al. (2025) Haplotype-based analysis distinguishes maternal-fetal genetic contribution to pregnancy-related outcomes. PLoS Genet 21(3): e1011575. https://doi.org/10.1371/journal.pgen.1011575
https://creativecommons.org/licenses/by/4.0/
© 2025 Srivastava et al. 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 credited.
https://creativecommons.org/licenses/by/4.0/
© 2025 Srivastava et al. 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 credited.
https://creativecommons.org/licenses/by/4.0/
Julkaisun pysyvä osoite on
https://urn.fi/URN:NBN:fi:oulu-202505153494
https://urn.fi/URN:NBN:fi:oulu-202505153494
Tiivistelmä
Abstract
Genotype-based approaches for the estimation of SNP-based narrow-sense heritability (\(\hat{\rm{h}}^2\)) have limited utility in pregnancy-related outcomes due to confounding by the shared alleles between mother and child. Here, we propose a haplotype-based approach to estimate the genetic variance attributable to three haplotypes - maternal transmitted (\(\hat{\rm{h}}^2_{\rm{m1}}\)), maternal non-transmitted (\(\hat{\rm{h}}^2_{\rm{m2}}\)) and paternal transmitted (\(\hat{\rm{h}}^2_{\rm{p1}}\)) in mother-child pairs. We show through extensive simulations that our haplotype-based approach outperforms the conventional and contemporary approaches for resolving the contribution of maternal and fetal effects, particularly when m1 and p1 have different effects in the offspring. We apply this approach to estimate the explicit and relative maternal-fetal genetic contribution to the phenotypic variance of gestational duration and gestational duration-adjusted fetal size measurements at birth in 10,375 mother-child pairs. The results reveal that variance of gestational duration is mainly attributable to m1 and m2 (\(\hat{\rm{h}}^2_{\rm{m1}}\) = 17.3%, S.E. = 5.2%, \(\hat{\rm{h}}^2_{\rm{m2}}\) = 12.3%, S.E. = 5.2%, \(\hat{\rm{h}}^2_{\rm{p1}}\) = 0.0%, S.E. = 5.0%). In contrast, variance of fetal size measurements at birth are mainly attributable to m1 and p1 (\(\hat{\rm{h}}^2_{\rm{m1}}\) = 18.6 − 36.4%, \(\hat{\rm{h}}^2_{\rm{m2}}\) = 0.0 − 5.2%, \(\hat{\rm{h}}^2_{\rm{p1}}\) = 4.4 − 13.6%). Our results suggest that gestational duration and fetal size measurements are primarily genetically determined by the maternal and fetal genomes, respectively. In addition, a greater contribution of m1 as compared to m2 and p1 (\(\hat{\rm{h}}^2_{\rm{m1}}\) − \(\hat{\rm{h}}^2_{\rm{m2}}\) − \(\hat{\rm{h}}^2_{\rm{p1}}\) > 0) to birth length and head circumference suggests a substantial influence of correlated maternal-fetal genetic effects on these traits. Our newly developed approach provides a direct and robust alternative for resolving explicit maternal and fetal genetic contributions to the phenotypic variance of pregnancy-related outcomes.
Genotype-based approaches for the estimation of SNP-based narrow-sense heritability (\(\hat{\rm{h}}^2\)) have limited utility in pregnancy-related outcomes due to confounding by the shared alleles between mother and child. Here, we propose a haplotype-based approach to estimate the genetic variance attributable to three haplotypes - maternal transmitted (\(\hat{\rm{h}}^2_{\rm{m1}}\)), maternal non-transmitted (\(\hat{\rm{h}}^2_{\rm{m2}}\)) and paternal transmitted (\(\hat{\rm{h}}^2_{\rm{p1}}\)) in mother-child pairs. We show through extensive simulations that our haplotype-based approach outperforms the conventional and contemporary approaches for resolving the contribution of maternal and fetal effects, particularly when m1 and p1 have different effects in the offspring. We apply this approach to estimate the explicit and relative maternal-fetal genetic contribution to the phenotypic variance of gestational duration and gestational duration-adjusted fetal size measurements at birth in 10,375 mother-child pairs. The results reveal that variance of gestational duration is mainly attributable to m1 and m2 (\(\hat{\rm{h}}^2_{\rm{m1}}\) = 17.3%, S.E. = 5.2%, \(\hat{\rm{h}}^2_{\rm{m2}}\) = 12.3%, S.E. = 5.2%, \(\hat{\rm{h}}^2_{\rm{p1}}\) = 0.0%, S.E. = 5.0%). In contrast, variance of fetal size measurements at birth are mainly attributable to m1 and p1 (\(\hat{\rm{h}}^2_{\rm{m1}}\) = 18.6 − 36.4%, \(\hat{\rm{h}}^2_{\rm{m2}}\) = 0.0 − 5.2%, \(\hat{\rm{h}}^2_{\rm{p1}}\) = 4.4 − 13.6%). Our results suggest that gestational duration and fetal size measurements are primarily genetically determined by the maternal and fetal genomes, respectively. In addition, a greater contribution of m1 as compared to m2 and p1 (\(\hat{\rm{h}}^2_{\rm{m1}}\) − \(\hat{\rm{h}}^2_{\rm{m2}}\) − \(\hat{\rm{h}}^2_{\rm{p1}}\) > 0) to birth length and head circumference suggests a substantial influence of correlated maternal-fetal genetic effects on these traits. Our newly developed approach provides a direct and robust alternative for resolving explicit maternal and fetal genetic contributions to the phenotypic variance of pregnancy-related outcomes.
Kokoelmat
- Avoin saatavuus [38506]
Ellei muuten mainita, aineiston lisenssi on https://creativecommons.org/licenses/by/4.0/