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Abstract
Prenatal alcohol exposure (PAE) can result in cognitive and behavioral disabilities and growth deficits. Because alcohol-related neurobehavioral deficits may occur in the absence of overt dysmorphic features or growth deficits, there is a need to identify biomarkers of PAE that can predict neurobehavioral impairment. In this study, we assessed infant plasma extracellular, circulating miRNAs (exmiRNAs) obtained from a heavily exposed Cape Town cohort to determine whether these can be used to predict PAE-related growth restriction and cognitive impairment. PAE, controlling for smoking as a covariate, altered 27% of expressed exmiRNAs with clinically-relevant effect sizes (Cohen’s d ≥ 0.4). Moreover, at 2 weeks, PAE increased correlated expression of exmiRNAs across chromosomes, suggesting potential co-regulation. In confirmatory factor analysis, the variance in expression for PAE-altered exmiRNAs at 2 weeks and 6.5 months was best described by three-factor models. Pathway analysis found that factors at 2 weeks were associated with (F1) cell maturation, cell cycle inhibition, and somatic growth, (F2) cell survival, apoptosis, cardiac development, and metabolism, and (F3) cell proliferation, skeletal development, hematopoiesis, and inflammation, and at 6.5 months with (F1) neurodevelopment, neural crest/mesoderm-derivative development and growth, (F2) immune system and inflammation, and (F3) somatic growth and cardiovascular development. Factors F3 at 2 weeks and F2 at 6.5 months partially mediated PAE-induced growth deficits, and factor F3 at 2 weeks partially mediated effects of PAE on infant recognition memory at 6.5 months. These findings indicate that infant exmiRNAs can help identify infants who will exhibit PAE-related deficits in growth and cognition.
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1 Texas A&M University Health Science Center, Department of Neuroscience and Experimental Therapeutics, Bryan, USA (GRID:grid.412408.b); Texas A&M University Health Science Center, Women’s Health in Neuroscience Program, Bryan, USA (GRID:grid.412408.b)
2 Institutional Centers for Clinical and Translational Research, Harvard Medical School, Boston Children’s Hospital, Boston, USA (GRID:grid.412408.b)
3 Texas A&M University Health Science Center, Department of Neuroscience and Experimental Therapeutics, Bryan, USA (GRID:grid.412408.b)
4 Columbia University Medical Center, Departments of Pediatrics and Emergency Medicine, Institute of Human Nutrition, New York, USA (GRID:grid.239585.0) (ISNI:0000 0001 2285 2675)
5 Wayne State University School of Medicine, Department of Psychiatry and Behavioral Neurosciences, Detroit, USA (GRID:grid.254444.7) (ISNI:0000 0001 1456 7807)
6 University of Cape Town, Departments of Human Biology and of Psychiatry and Mental Health, Faculty of Health Sciences, Cape Town, South Africa (GRID:grid.7836.a) (ISNI:0000 0004 1937 1151)
7 University of Cape Town, Division of Biomedical Engineering, Department of Human Biology, Faculty of Health Sciences, Cape Town, South Africa (GRID:grid.7836.a) (ISNI:0000 0004 1937 1151)
8 Wayne State University School of Medicine, Department of Psychiatry and Behavioral Neurosciences, Detroit, USA (GRID:grid.254444.7) (ISNI:0000 0001 1456 7807); University of Cape Town, Departments of Human Biology and of Psychiatry and Mental Health, Faculty of Health Sciences, Cape Town, South Africa (GRID:grid.7836.a) (ISNI:0000 0004 1937 1151)