Maternal polymorphisms in glutathione-related genes are associated with maternal mercury concentrations and early child neurodevelopment in a population with a fish-rich diet.

Journal: Environment international

Volume: 115

Issue: 

Year of Publication: 2019

Affiliated Institutions:  Department of Laboratory Medicine, Division of Occupational and Environmental Medicine, Lund University, Lund, Sweden. University of Rochester Medical Center, School of Medicine and Dentistry, Elmwood Ave, Rochester, NY , USA. Nutrition Innovation Centre for Food and Health (NICHE), Ulster University, Cromore Road, Coleraine BT SA, Co. Londonderry, UK. The Child Development Centre, Ministry of Health, Mahé, Seychelles. Department of Laboratory Medicine, Division of Occupational and Environmental Medicine, Lund University, Lund, Sweden; Institute of Environmental Medicine, Metals and Health, Box , Stockholm, Sweden. Electronic address: karin.broberg@ki.se.

Abstract summary 

Glutathione (GSH) pathways play a key role the metabolism and elimination of the neurotoxicant methylmercury (MeHg). We hypothesized that maternal genetic variation linked to GSH pathways could influence MeHg concentrations in pregnant mothers and children and thereby also affect early life development.The GCLM (rs41303970, C/T), GCLC (rs761142, T/G) and GSTP1 (rs1695, A/G) polymorphisms were genotyped in 1449 mothers in a prospective study of the Seychellois population with a diet rich in fish. Genotypes were analyzed in association with maternal hair and blood Hg, fetal blood Hg (cord blood Hg), as well as children's mental (MDI) and motor development (PDI; MDI and PDI assessed by Bayley Scales of Infant Development at 20 months). We also examined whether genotypes modified the association between Hg exposure and developmental outcomes.GCLC rs761142 TT homozygotes showed statistically higher mean maternal hair Hg (4.12 ppm) than G carriers (AG 3.73 and GG 3.52 ppm) (p = 0.037). For the combination of GCLC rs761142 and GCLM rs41303970, double homozygotes TT + CC showed higher hair Hg (4.40 ppm) than G + T carriers (3.44 ppm; p = 0.018). No associations were observed between GSTP1 rs1695 and maternal hair Hg or between any genotypes and maternal blood Hg or cord blood Hg. The maternal GSTP1 rs1695 rare allele (G) was associated with a lower MDI among children (β = -1.48, p = 0.048). We also observed some interactions: increasing Hg in maternal and cord blood was associated with lower PDI among GCLC rs761142 TT carriers; and increasing Hg in hair was associated with lower MDI among GSTP1 rs1695 GG carriers.Maternal genetic variation in genes involved in GSH synthesis is statistically associated with Hg concentrations in maternal hair, but not in maternal or fetal blood. We observed interactions that suggest maternal GSH genetics may modify associations between MeHg exposure and neurodevelopmental outcomes.

Authors & Co-authors:  Wahlberg Karin K Love Tanzy M TM Pineda Daniela D Engström Karin K Watson Gene E GE Thurston Sally W SW Yeates Alison J AJ Mulhern Maria S MS McSorley Emeir M EM Strain J J JJ Smith Tristram H TH Davidson Philip W PW Shamlaye Conrad F CF Myers G J GJ Rand Matthew D MD van Wijngaarden Edwin E Broberg Karin K

Study Outcome 

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Citations :  Ali-Osman F, Akande O, Antoun G, et al. Molecular cloning, characterization, and expression in Escherichia coli of full-length cDNAs of three human glutathione S-transferase Pi gene variants Evidence for differential catalytic activity of the encoded proteins. J Biol Chem. 1997;272:10004–10012.
Authors :  17
Identifiers
Doi : 10.1016/j.envint.2018.03.015
SSN : 1873-6750
Study Population
Mothers
Mesh Terms
Animals
Other Terms
GCLC;GCLM;GSTP1;Methylmercury;Neurodevelopment
Study Design
Study Approach
Country of Study
Publication Country
Netherlands