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161. Maternal Glucocorticoid Metabolism Across Pregnancy: A Potential Mechanism Underlying Fetal Glucocorticoid Exposure

Author

Stoye, David Q, primary, Andrew, Ruth, additional, Grobman, William A, additional, Adam, Emma K, additional, Wadhwa, Pathik D, additional, Buss, Claudia, additional, Entringer, Sonja, additional, Miller, Gregory E, additional, Boardman, James P, additional, Seckl, Jonathan R, additional, Keenan-Devlin, Lauren S, additional, Borders, Ann E B, additional, and Reynolds, Rebecca M, additional

Published
2020
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164. A Role of Oxytocin Receptor Gene Brain Tissue Expression Quantitative Trait Locus rs237895 in the Intergenerational Transmission of the Effects of Maternal Childhood Maltreatment

Author

Toepfer, Philipp, primary, O'Donnell, Kieran J., additional, Entringer, Sonja, additional, Heim, Christine M., additional, Lin, David T.S., additional, MacIsaac, Julia L., additional, Kobor, Michael S., additional, Meaney, Michael J., additional, Provençal, Nadine, additional, Binder, Elisabeth B., additional, Wadhwa, Pathik D., additional, and Buss, Claudia, additional

Published
2019
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171. Rate of Gestational Weight Gain and Glucose- Insulin Metabolism Among Hispanic Pregnant Women With Overweight and Obesity.

Author

Lindsay, Karen L., Gyllenhammer, Lauren E., Entringer, Sonja, and Wadhwa, Pathik D.

Subjects
WEIGHT gain, GLUCOSE, PREGNANT women
Abstract

Context: Hispanic women are at elevated risk of gestational glucose intolerance and postpartum type 2 diabetes compared with non-Hispanic White women. Identification of potentially modifiable factors contributing to this trajectory of beta-cell dysfunction is warranted. Objective: We aimed to determine the association between rate of gestational weight gain (rGWG) and glucose-insulin metabolism in Hispanic pregnant women with overweight and obesity. Methods: This cross-sectional, observational study, conducted from 2018-2020 at the clinical research center at University of California, Irvine, included 33 nondiabetic Hispanic pregnant women at 28 to 30 weeks’ gestation with pre-pregnancy body mass index (BMI) 25.0 to 34.9 kg/m2. Participants consumed a standardized liquid mixed meal after an overnight fast. Serial blood samples were collected at fasting and up to 2 hours postprandial. The glucose and insulin area under the curve (AUC), insulin sensitivity index (ISI) and insulin secretion sensitivity index (ISSI)-2 were computed. Context: Hispanic women are at elevated risk of gestational glucose intolerance and postpartum type 2 diabetes compared with non-Hispanic White women. Identification of potentially modifiable factors contributing to this trajectory of beta-cell dysfunction is warranted. Objective: We aimed to determine the association between rate of gestational weight gain (rGWG) and glucose-insulin metabolism in Hispanic pregnant women with overweight and obesity. Methods: This cross-sectional, observational study, conducted from 2018-2020 at the clinical research center at University of California, Irvine, included 33 nondiabetic Hispanic pregnant women at 28 to 30 weeks’ gestation with pre-pregnancy body mass index (BMI) 25.0 to 34.9 kg/m2. Participants consumed a standardized liquid mixed meal after an overnight fast. Serial blood samples were collected at fasting and up to 2 hours postprandial. The glucose and insulin area under the curve (AUC), insulin sensitivity index (ISI) and insulin secretion sensitivity index (ISSI)-2 were computed. [ABSTRACT FROM AUTHOR]

Published
2022
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172. Early development of negative and positive affect: Implications for ADHD symptomatology across three birth cohorts.

Author

Gustafsson, Hanna C., Nolvi, Saara, Sullivan, Elinor L., Rasmussen, Jerod M., Gyllenhammer, Lauren E., Entringer, Sonja, Wadhwa, Pathik D., O'Connor, Thomas G., Karlsson, Linnea, Karlsson, Hasse, Korja, Riikka, Buss, Claudia, Graham, Alice M., and Nigg, Joel T.

Subjects
AFFECT (Psychology), ATTENTION-deficit hyperactivity disorder, SYMPTOMS, INFANTS
Abstract

High levels of early emotionality (of either negative or positive valence) are hypothesized to be important precursors to early psychopathology, with attention-deficit/hyperactivity disorder (ADHD) a prime early target. The positive and negative affect domains are prime examples of Research Domain Criteria (RDoC) concepts that may enrich a multilevel mechanistic map of psychopathology risk. Utilizing both variable-centered and person-centered approaches, the current study examined whether levels and trajectories of infant negative and positive emotionality, considered either in isolation or together, predicted children's ADHD symptoms at 4 to 8 years of age. In variable-centered analyses, higher levels of infant negative affect (at as early as 3 months of age) were associated with childhood ADHD symptoms. Findings for positive affect failed to reach statistical threshold. Results from person-centered trajectory analyses suggest that additional information is gained by simultaneously considering the trajectories of positive and negative emotionality. Specifically, only when exhibiting moderate, stable or low levels of positive affect did negative affect and its trajectory relate to child ADHD symptoms. These findings add to a growing literature that suggests that infant negative emotionality is a promising early life marker of future ADHD risk and suggest secondarily that moderation by positive affectivity warrants more consideration. [ABSTRACT FROM AUTHOR]

Published
2021
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173. Dynamic DNA methylation changes in the maternal oxytocin gene locus (OXT) during pregnancy predict postpartum maternal intrusiveness

Author

Toepfer, Philipp, O'Donnell, Kieran J, Entringer, Sonja, Garg, Elika, Heim, Christine M, Lin, David TS, MacIsaac, Julia L, Kobor, Michael S, Meaney, Michael J, Provençal, Nadine, Binder, Elisabeth B, Wadhwa, Pathik D, and Buss, Claudia

Subjects
Adult, Male, Reproductive health and childbirth, Oxytocin, Medical and Health Sciences, Promoter Regions, Genetic, Postpartum, Pregnancy, Receptors, Genetics, Humans, Maternal behavior, Maternal Behavior, Pediatric, Psychiatry, DNA methylation, Depression, Estrogen sensitivity, Postpartum Period, Psychology and Cognitive Sciences, Infant, DNA Methylation, Newborn, Mother-Child Relations, Behavioral epigenetics, Good Health and Well Being, Female, Epigenesis
Abstract

Maternal behavior (MB) is observable across mammals and represents an important feature of environmental variation during early postnatal development. Oxytocin (OT) plays a crucial role in MB. Even prior to childbirth, pregnancy induces epigenetic and other downstream changes in the maternal OT-system, likely mediated by the actions of steroid hormones. However, little is known about the nature and consequences of epigenetic modifications in the maternal OT-encoding gene (OXT) during pregnancy. Our study aims to investigate temporal dynamics of OXT promoter DNA methylation (DNAm) throughout pregnancy in predicting MB in humans. In 107 mother-child dyads, maternal OXT DNAm was serially analyzed in whole blood in early, mid and late pregnancy. MB was coded based on standardized mother-child interactions at six months postpartum. After controlling for cellular heterogeneity, race/ethnicity, age, and socioeconomic status, OXT-promoter DNAm exhibited a dynamic profile during pregnancy (b = 0.026, t=-3.37, p

Published
2019

174. Integrated analysis of environmental and genetic influences on cord blood DNA methylation in new-borns

Author

Czamara, Darina, Eraslan, Gökçen, Page, Christian M., Lahti, Jari, Lahti-Pulkkinen, Marius, Hämäläinen, Esa, Kajantie, Eero, Laivuori, Hannele, Villa, Pia M., Reynolds, Rebecca M., Nystad, Wenche, Håberg, Siri E., London, Stephanie J., O’Donnell, Kieran J., Garg, Elika, Meaney, Michael J., Entringer, Sonja, Wadhwa, Pathik D., Buss, Claudia, Jones, Meaghan J., Lin, David T. S., MacIsaac, Julie L., Kobor, Michael S., Koen, Nastassja, Zar, Heather J., Koenen, Karestan C., Dalvie, Shareefa, Stein, Dan J., Kondofersky, Ivan, Müller, Nikola S., Theis, Fabian J., Wray, Naomi R., Ripke, Stephan, Mattheisen, Manuel, Trzaskowski, Maciej, Byrne, Enda M., Abdellaoui, Abdel, Adams, Mark J., Agerbo, Esben, Air, Tracy M., Andlauer, Till F. M., Bacanu, Silviu-Alin, Bækvad-Hansen, Marie, Beekman, Aartjan T. F., Bigdeli, Tim B., Blackwood, Douglas H. R., Bryois, Julien, Buttenschøn, Henriette N., Bybjerg-Grauholm, Jonas, Cai, Na, Castelao, Enrique, Christensen, Jane Hvarregaard, Clarke, Toni-Kim, Coleman, Jonathan R. I., Colodro-Conde, Lucía, Couvy-Duchesne, Baptiste, Craddock, Nick, Crawford, Gregory E., Davies, Gail, Deary, Ian J., Degenhardt, Franziska, Derks, Eske M., Direk, Nese, Dolan, Conor V., Dunn, Erin C., Eley, Thalia C., Escott-Price, Valentina, Kiadeh, Farnush Farhadi Hassan, Finucane, Hilary K., Forstner, Andreas J., Frank, Josef, Gaspar, Héléna A., Gill, Michael, Goes, Fernando S., Gordon, Scott D., Grove, Jakob, Hall, Lynsey S., Hansen, Christine Søholm, Hansen, Thomas F., Herms, Stefan, Hickie, Ian B., Hoffmann, Per, Homuth, Georg, Horn, Carsten, Hottenga, Jouke-Jan, Hougaard, David M., Ising, Marcus, Jansen, Rick, Jorgenson, Eric, Knowles, James A., Kohane, Isaac S., Kraft, Julia, Kretzschmar, Warren W., Krogh, Jesper, Kutalik, Zoltán, Li, Yihan, Lind, Penelope A., MacIntyre, Donald J., MacKinnon, Dean F., Maier, Robert M., Maier, Wolfgang, Marchini, Jonathan, Mbarek, Hamdi, McGrath, Patrick, McGuffin, Peter, Medland, Sarah E., Mehta, Divya, Middeldorp, Christel M., Mihailov, Evelin, Milaneschi, Yuri, Milani, Lili, Mondimore, Francis M., Montgomery, Grant W., Mostafavi, Sara, Mullins, Niamh, Nauck, Matthias, Ng, Bernard, Nivard, Michel G., Nyholt, Dale R., O’Reilly, Paul F., Oskarsson, Hogni, Owen, Michael J., Painter, Jodie N., Pedersen, Carsten Bøcker, Pedersen, Marianne Giørtz, Peterson, Roseann E., Pettersson, Erik, Peyrot, Wouter J., Pistis, Giorgio, Posthuma, Danielle, Quiroz, Jorge A., Qvist, Per, Rice, John P., Riley, Brien P., Rivera, Margarita, Mirza, Saira Saeed, Schoevers, Robert, Schulte, Eva C., Shen, Ling, Shi, Jianxin, Shyn, Stanley I., Sigurdsson, Engilbert, Sinnamon, Grant C. B., Smit, Johannes H., Smith, Daniel J., Stefansson, Hreinn, Steinberg, Stacy, Streit, Fabian, Strohmaier, Jana, Tansey, Katherine E., Teismann, Henning, Teumer, Alexander, Thompson, Wesley, Thomson, Pippa A., Thorgeirsson, Thorgeir E., Traylor, Matthew, Treutlein, Jens, Trubetskoy, Vassily, Uitterlinden, André G., Umbricht, Daniel, Van der Auwera, Sandra, van Hemert, Albert M., Viktorin, Alexander, Visscher, Peter M., Wang, Yunpeng, Webb, Bradley T., Weinsheimer, Shantel Marie, Wellmann, Jürgen, Willemsen, Gonneke, Witt, Stephanie H., Wu, Yang, Xi, Hualin S., Yang, Jian, Zhang, Futao, Arolt, Volker, Baune, Bernhard T., Berger, Klaus, Boomsma, Dorret I., Cichon, Sven, Dannlowski, Udo, de Geus, E. J. C., DePaulo, J. Raymond, Domenici, Enrico, Domschke, Katharina, Esko, Tõnu, Grabe, Hans J., Hamilton, Steven P., Hayward, Caroline, Heath, Andrew C., Kendler, Kenneth S., Kloiber, Stefan, Lewis, Glyn, Li, Qingqin S., Lucae, Susanne, Madden, Pamela A. F., Magnusson, Patrik K., Martin, Nicholas G., McIntosh, Andrew M., Metspalu, Andres, Mors, Ole, Mortensen, Preben Bo, Müller-Myhsok, Bertram, Nordentoft, Merete, Nöthen, Markus M., O’Donovan, Michael C., Paciga, Sara A., Pedersen, Nancy L., Penninx, Brenda W. J. H., Perlis, Roy H., Porteous, David J., Potash, James B., Preisig, Martin, Rietschel, Marcella, Schaefer, Catherine, Schulze, Thomas G., Smoller, Jordan W., Stefansson, Kari, Tiemeier, Henning, Uher, Rudolf, Völzke, Henry, Weissman, Myrna M., Werge, Thomas, Lewis, Cathryn M., Levinson, Douglas F., Breen, Gerome, Børglum, Anders D., Sullivan, Patrick F., Räikkönen, Katri, Binder, Elisabeth B., Consortium, Major Depressive Disorder Working Group of the Psychiatric Genomics, Epidemiology, Internal Medicine, Child and Adolescent Psychiatry / Psychology, Psychiatry, APH - Mental Health, Human genetics, Amsterdam Reproduction & Development (AR&D), APH - Methodology, APH - Digital Health, Department of Psychology and Logopedics, Helsinki Collegium for Advanced Studies, Faculty of Medicine, Developmental Psychology Research Group, Medicum, HUSLAB, Department of Diagnostics and Therapeutics, HUS Children and Adolescents, Lastentautien yksikkö, Children's Hospital, HUS Gynecology and Obstetrics, Institute for Molecular Medicine Finland, Pregnancy and Genes, Department of Medical and Clinical Genetics, Department of Obstetrics and Gynecology, Helsinki Institute of Life Science HiLIFE, Genomics of Neurological and Neuropsychiatric Disorders, Biological Psychology, APH - Health Behaviors & Chronic Diseases, APH - Personalized Medicine, Complex Trait Genetics, Amsterdam Neuroscience - Complex Trait Genetics, Interdisciplinary Centre Psychopathology and Emotion regulation (ICPE), Perceptual and Cognitive Neuroscience (PCN), Clinical Cognitive Neuropsychiatry Research Program (CCNP), Adult Psychiatry, Major Depressive Disorder Working Group of the Psychiatric Genomics Consortium, Wray, N.R., Ripke, S., Mattheisen, M., Trzaskowski, M., Byrne, E.M., Abdellaoui, A., Adams, M.J., Agerbo, E., Air, T.M., Andlauer, TFM, Bacanu, S.A., Bækvad-Hansen, M., Beekman, ATF, Bigdeli, T.B., Blackwood, DHR, Bryois, J., Buttenschøn, H.N., Bybjerg-Grauholm, J., Cai, N., Castelao, E., Christensen, J.H., Clarke, T.K., Coleman, JRI, Colodro-Conde, L., Couvy-Duchesne, B., Craddock, N., Crawford, G.E., Davies, G., Deary, I.J., Degenhardt, F., Derks, E.M., Direk, N., Dolan, C.V., Dunn, E.C., Eley, T.C., Escott-Price, V., Kiadeh, FFH, Finucane, H.K., Forstner, A.J., Frank, J., Gaspar, H.A., Gill, M., Goes, F.S., Gordon, S.D., Grove, J., Hall, L.S., Hansen, C.S., Hansen, T.F., Herms, S., Hickie, I.B., Hoffmann, P., Homuth, G., Horn, C., Hottenga, J.J., Hougaard, D.M., Ising, M., Jansen, R., Jorgenson, E., Knowles, J.A., Kohane, I.S., Kraft, J., Kretzschmar, W.W., Krogh, J., Kutalik, Z., Li, Y., Lind, P.A., MacIntyre, D.J., MacKinnon, D.F., Maier, R.M., Maier, W., Marchini, J., Mbarek, H., McGrath, P., McGuffin, P., Medland, S.E., Mehta, D., Middeldorp, C.M., Mihailov, E., Milaneschi, Y., Milani, L., Mondimore, F.M., Montgomery, G.W., Mostafavi, S., Mullins, N., Nauck, M., Ng, B., Nivard, M.G., Nyholt, D.R., O'Reilly, P.F., Oskarsson, H., Owen, M.J., Painter, J.N., Pedersen, C.B., Pedersen, M.G., Peterson, R.E., Pettersson, E., Peyrot, W.J., Pistis, G., Posthuma, D., Quiroz, J.A., Qvist, P., Rice, J.P., Riley, B.P., Rivera, M., Mirza, S.S., Schoevers, R., Schulte, E.C., Shen, L., Shi, J., Shyn, S.I., Sigurdsson, E., Sinnamon, GCB, Smit, J.H., Smith, D.J., Stefansson, H., Steinberg, S., Streit, F., Strohmaier, J., Tansey, K.E., Teismann, H., Teumer, A., Thompson, W., Thomson, P.A., Thorgeirsson, T.E., Traylor, M., Treutlein, J., Trubetskoy, V., Uitterlinden, A.G., Umbricht, D., Van der Auwera, S., van Hemert, A.M., Viktorin, A., Visscher, P.M., Wang, Y., Webb, B.T., Weinsheimer, S.M., Wellmann, J., Willemsen, G., Witt, S.H., Wu, Y., Xi, H.S., Yang, J., Zhang, F., Arolt, V., Baune, B.T., Berger, K., Boomsma, D.I., Cichon, S., Dannlowski, U., de Geus, EJC, DePaulo, J.R., Domenici, E., Domschke, K., Esko, T., Grabe, H.J., Hamilton, S.P., Hayward, C., Heath, A.C., Kendler, K.S., Kloiber, S., Lewis, G., Li, Q.S., Lucae, S., Madden, PAF, Magnusson, P.K., Martin, N.G., McIntosh, A.M., Metspalu, A., Mors, O., Mortensen, P.B., Müller-Myhsok, B., Nordentoft, M., Nöthen, M.M., O'Donovan, M.C., Paciga, S.A., Pedersen, N.L., Penninx, BWJH, Perlis, R.H., Porteous, D.J., Potash, J.B., Preisig, M., Rietschel, M., Schaefer, C., Schulze, T.G., Smoller, J.W., Stefansson, K., Tiemeier, H., Uher, R., Völzke, H., Weissman, M.M., Werge, T., Lewis, C.M., Levinson, D.F., Breen, G., Børglum, A.D., Sullivan, P.F., Læknadeild (HÍ), Faculty of Medicine (UI), Heilbrigðisvísindasvið (HÍ), School of Health Sciences (UI), Háskóli Íslands, and University of Iceland

Subjects
Male, Epigenomics, 0301 basic medicine, Netherlands Twin Register (NTR), Erfðagreining, General Physics and Astronomy, Genome-wide association study, 02 engineering and technology, Major Depressive Disorder Working Group of the Psychiatric Genomics Consortium, Epigenesis, Genetic, Cohort Studies, PRENATAL STRESS, Pregnancy, Risk Factors, Genamengi, Genotype, 2.1 Biological and endogenous factors, MATERNAL SMOKING, Aetiology, Gene–environment interaction, lcsh:Science, 10. No inequality, Pediatric, RISK, Genetics, DNA methylation, Multidisciplinary, 1184 Genetics, developmental biology, physiology, Methylation, Fetal Blood, 021001 nanoscience & nanotechnology, GENOTYPE, ddc, 3. Good health, PREGNANCY, Nýburar, Female, ddc:500, 0210 nano-technology, BIRTH, Science, IN-UTERO, Biology, CHILDHOOD MALTREATMENT, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Genetic, MD Multidisciplinary, Humans, Epigenetics, Prevention, Human Genome, NORWEGIAN MOTHER, GENOME-WIDE, Infant, Newborn, Infant, biomarkers, dNaM, DNA, General Chemistry, Newborn, DNA-rannsóknir, 030104 developmental biology, epigenomics, lcsh:Q, Gene-Environment Interaction, 3111 Biomedicine, Biomarkers, Epigenesis
Abstract

Publisher's version (útgefin grein), Epigenetic processes, including DNA methylation (DNAm), are among the mechanisms allowing integration of genetic and environmental factors to shape cellular function. While many studies have investigated either environmental or genetic contributions to DNAm, few have assessed their integrated effects. Here we examine the relative contributions of prenatal environmental factors and genotype on DNA methylation in neonatal blood at variably methylated regions (VMRs) in 4 independent cohorts (overall n = 2365). We use Akaike’s information criterion to test which factors best explain variability of methylation in the cohort-specific VMRs: several prenatal environmental factors (E), genotypes in cis (G), or their additive (G + E) or interaction (GxE) effects. Genetic and environmental factors in combination best explain DNAm at the majority of VMRs. The CpGs best explained by either G, G + E or GxE are functionally distinct. The enrichment of genetic variants from GxE models in GWAS for complex disorders supports their importance for disease risk., We want to thank Susanne Sauer and Maik Ködel for their technical assistance and Jessica Keverne for language editing. We thank all mothers who took part in the on-going PREDO study. We are grateful to all the families in Norway who participate in the on-going MoBa cohort study. We thank the Drakenstein Child Health Study staff, and the clinical and administrative staff of the Western Cape Government Department of Health at Paarl Hospital and at the clinics for support of the Study. We also thank our collaborators and students. Finally, we thank all mothers and children enroled in the Drakenstein Child Health Study. We thank the research participants and employees of 23andMe, Inc. for their contribution to this study. This work was supported by the Academy of Finland (E.K., H.L., K.R., and J.L.); University of Helsinki Research Funds (J.L., M.L.P., and H.L.), British Heart Foundation (RMR); Tommy’s (RMR); European Commission (EK, KR, Horizon 2020 Award SC1–2016-RTD-733280 RECAP); NorFace DIAL (E.K., KR PremLife); Foundation for Pediatric Research (E.K.); Juho Vainio Foundation (E.K.); Novo Nordisk Foundation (E.K.); Signe and Ane Gyllenberg Foundation (E.K., K.R.); Sigrid Jusélius Foundation (E.K.); Finnish Medical Foundation (H.L.); Jane and Aatos Erkko Foundation (H.L.); Päivikki and Sakari Sohlberg Foundation (H.L., P.M.V.); the Clinical Graduate school in Pediatrics and Obstetrics/Gynaecology in University of Helsinki (P.M.V.). The Norwegian Mother and Child Cohort Study is supported by the Norwegian Ministry of Health and Care Services and the Ministry of Education and Research, NIH/NIEHS (contract no N01-ES-75558), NIH/NINDS (grant no.1 UO1 NS 047537–01 and grant no.2 UO1 NS 047537–06A1). For this work, MoBa 1 and 2 were supported by the Intramural Research Program of the NIH, National Institute of Environmental Health Sciences (Z01-ES-49019) and the Norwegian Research Council/BIOBANK (grant no 221097). This work was also partly supported by the Research Council of Norway through its Centres of Excellence funding scheme, project number 262700. The Drakenstein Child Health Study is supported by the Bill and Melinda Gates Foundation (OPP 1017641); with additional support for this work from the Eunice Kennedy Shriver National Institute of Child Health and Human Development of the National Institutes of Health (NICHD) under Award Number R21HD085849; and the Fogarty International Center (FIC). The content is solely the responsibility of the authors and does not necessarily represent the official views of the National Institutes of Health. Additional support for H.J.Z., D.J.S. and N.K., and for research reported in this publication was by the South African Medical Research Council (SAMRC); N.K. receives support from the SAMRC under a Self-Initiated Research Grant. The views and opinions expressed are those of the authors and do not necessarily represent the official views of the SAMRC. This work was also funded by the German Federal Ministry of Education and Research through the Research Consortium Integrated Network IntegraMent (grant 01ZX1314H) under the auspices of the e:Med Programme (NSM). The UCI cohort was supported by a European Research Area Network (ERA Net) Neuron grant (01EW1407A, CB) and National Institutes of Health grant (R01 HD-060628, CB) as well as NIH grant R01 MH-105538 (PDW). This work was also funded by the Canadian Institute for Advanced Research, Child and Brain Development Program, Toronto, ON, Canada (KJOD).

Published
2019

175. Antenatal depression, psychotropic medication use, and inflammation among pregnant women

Author

Miller, Emily S, Grobman, William A, Culhane, Jennifer, Adam, Emma, Buss, Claudia, Entringer, Sonja, Miller, Gregory, Wadhwa, Pathik D, Keenan-Devlin, Lauren, and Borders, Ann

Subjects
Adult, Pregnancy, Clinical Research, Selective serotonin reuptake inhibitors, Humans, Psychology, Inflammation, Psychiatric Status Rating Scales, Psychiatry, Psychotropic Drugs, Antenatal depression, Tumor Necrosis Factor-alpha, Depression, Evaluation of treatments and therapeutic interventions, Perinatal depression, United States, Brain Disorders, Pregnancy Complications, Cross-Sectional Studies, Mental Health, Anti-depressants, 6.1 Pharmaceuticals, Female, Cognitive Sciences, Pregnant Women, Drug Monitoring, Biomarkers
Abstract

To evaluate the association between psychotropic medication and inflammatory biomarkers in women with antenatal depressive symptoms (ADS). In this cross-sectional secondary analysis of a prospective multicenter observational study, 723 pregnant women underwent a depression screen using the Center for Epidemiologic Studies Depression Scale (CES-D) between 12 and 21weeks gestation. Self-reported use of medications for depression and/or anxiety was corroborated with the medical record to document exposure to pharmacotherapy. Serum was collected and inflammatory biomarkers (IFNγ, IL13, IL6, IL8, TNFα, CRP) were measured concomitantly. Women were included if they fell into one of three categories: ADS responsive to treatment (CES-D

Published
2018

177. Neonatal White Matter Maturation Is Associated With Infant Language Development.

Author

Sket, Georgina M, Sket, Georgina M, Overfeld, Judith, Styner, Martin, Gilmore, John H, Entringer, Sonja, Wadhwa, Pathik D, Rasmussen, Jerod M, Buss, Claudia, Sket, Georgina M, Sket, Georgina M, Overfeld, Judith, Styner, Martin, Gilmore, John H, Entringer, Sonja, Wadhwa, Pathik D, Rasmussen, Jerod M, and Buss, Claudia

Abstract

BackgroundWhile neonates have no sophisticated language skills, the neural basis for acquiring this function is assumed to already be present at birth. Receptive language is measurable by 6 months of age and meaningful speech production by 10-18 months of age. Fiber tracts supporting language processing include the corpus callosum (CC), which plays a key role in the hemispheric lateralization of language; the left arcuate fasciculus (AF), which is associated with syntactic processing; and the right AF, which plays a role in prosody and semantics. We examined if neonatal maturation of these fiber tracts is associated with receptive language development at 12 months of age.MethodsDiffusion-weighted imaging (DWI) was performed in 86 infants at 26.6 ± 12.2 days post-birth. Receptive language was assessed via the MacArthur-Bates Communicative Development Inventory at 12 months of age. Tract-based fractional anisotropy (FA) was determined using the NA-MIC atlas-based fiber analysis toolkit. Associations between neonatal regional FA, adjusted for gestational age at birth and age at scan, and language development at 12 months of age were tested using ANOVA models.ResultsAfter multiple comparisons correction, higher neonatal FA was positively associated with receptive language at 12 months of age within the genu (p < 0.001), rostrum (p < 0.001), and tapetum (p < 0.001) of the CC and the left fronto-parietal AF (p = 0.008). No significant clusters were found in the right AF.ConclusionMicrostructural development of the CC and the AF in the newborn is associated with receptive language at 12 months of age, demonstrating that interindividual variation in white matter microstructure is relevant for later language development, and indicating that the neural foundation for language processing is laid well ahead of the majority of language acquisition. This suggests that some origins of impaired language development may lie in the intrauterine and potentially neonatal perio

Published
2019

178. Maternal Interleukin-6 concentration during pregnancy is associated with variation in frontolimbic white matter and cognitive development in early life.

Author

Rasmussen, Jerod M, Rasmussen, Jerod M, Graham, Alice M, Entringer, Sonja, Gilmore, John H, Styner, Martin, Fair, Damien A, Wadhwa, Pathik D, Buss, Claudia, Rasmussen, Jerod M, Rasmussen, Jerod M, Graham, Alice M, Entringer, Sonja, Gilmore, John H, Styner, Martin, Fair, Damien A, Wadhwa, Pathik D, and Buss, Claudia

Abstract

Maternal inflammation during pregnancy can alter the trajectory of fetal brain development and increase risk for offspring psychiatric disorders. However, the majority of relevant research to date has been conducted in animal models. Here, in humans, we focus on the structural connectivity of frontolimbic circuitry as it is both critical for socioemotional and cognitive development, and commonly altered in a range of psychiatric disorders associated with intrauterine inflammation. Specifically, we test the hypothesis that elevated maternal concentration of the proinflammatory cytokine interleukin-6 (IL-6) during pregnancy will be associated with variation in microstructural properties of this circuitry in the neonatal period and across the first year of life. Pregnant mothers were recruited in early pregnancy and maternal blood samples were obtained for assessment of maternal IL-6 concentrations in early (12.6 ± 2.8 weeks [S.D.]), mid (20.4 ± 1.5 weeks [S.D.]) and late (30.3 ± 1.3 weeks [S.D.]) gestation. Offspring brain MRI scans were acquired shortly after birth (N = 86, scan age = 3.7 ± 1.7 weeks [S.D.]) and again at 12-mo age (N = 32, scan age = 54.0 ± 3.1 weeks [S.D.]). Diffusion Tensor Imaging (DTI) was used to characterize fractional anisotropy (FA) along the left and right uncinate fasciculus (UF), representing the main frontolimbic fiber tract. In N = 30 of the infants with serial MRI data at birth and 12-mo age, cognitive and socioemotional developmental status was characterized using the Bayley Scales of Infant Development. All analyses tested for potentially confounding influences of household income, prepregnancy Body-Mass-Index, obstetric risk, smoking during pregnancy, and infant sex, and outcomes at 12-mo age were additionally adjusted for the quality of the postnatal caregiving environment. Maternal IL-6 concentration (averaged across pregnancy) was prospectively and inversely associated with FA (suggestive of reduced integrity under high inflammato

Published
2019

179. Maternal Metabolomic Profile and Fetal Programming of Offspring Adiposity: Identification of Potentially Protective Lipid Metabolites.

Author

Hellmuth, Christian, Hellmuth, Christian, Lindsay, Karen L, Uhl, Olaf, Buss, Claudia, Wadhwa, Pathik D, Koletzko, Berthold, Entringer, Sonja, Hellmuth, Christian, Hellmuth, Christian, Lindsay, Karen L, Uhl, Olaf, Buss, Claudia, Wadhwa, Pathik D, Koletzko, Berthold, and Entringer, Sonja

Abstract

ScopeThe fetal programming paradigm posits that the origins of obesity can be traced, in part, to the intrauterine period of life. However, the mechanisms underlying fetal programming are not well understood, and few studies have measured offspring adiposity in the neonatal period. The aim of this study is to identify maternal metabolites, and their determinants, that are associated with neonatal adiposity.Methods and resultsA targeted metabolomics approach is applied to analyze plasma samples collected across gestation from a well-characterized cohort of 253 pregnant women participating in a prospective study at the University of California, Irvine. Whole-body dual X-ray absorptiometry (DXA) imaging of body composition is obtained in N = 121 newborns. Statistical models are adjusted for potential confounders and multiple testing. The authors identify six alkyl-linked phosphatidylcholines (PCae), containing fatty acid 20:4, that are significantly and negatively associated with neonatal body fat percentage. Factors indicating higher socioeconomic status, non-Hispanic ethnicity, and higher nonesterified fatty acid percentages are positively associated with these PCae.ConclusionsThe polyunsaturated fatty acid 20:4 contained in PCae may exert a beneficial effect with respect to future propensity for obesity development. Prepregnancy and early pregnancy factors are determinants of these PCae, highlighting the importance of addressing preconceptional conditions for fetal programming of newborn adiposity.

Published
2019

180. The Interplay Between Nutrition and Stress in Pregnancy: Implications for Fetal Programming of Brain Development.

Author

Lindsay, Karen L, Lindsay, Karen L, Buss, Claudia, Wadhwa, Pathik D, Entringer, Sonja, Lindsay, Karen L, Lindsay, Karen L, Buss, Claudia, Wadhwa, Pathik D, and Entringer, Sonja

Abstract

Growing evidence supports an important role for the intrauterine environment in shaping fetal development and subsequent child health and disease risk. The fetal brain is particularly plastic, whereby even subtle changes in structure and function produced by in utero conditions can have long-term implications. Based on the consideration that conditions related to energy substrate and likelihood of survival to reproductive age are particularly salient drivers of fetal programming, maternal nutrition and stress represent the most commonly, but independently, studied factors in this context. However, the effects of maternal nutrition and stress are context dependent and may be moderated by one another. Studies examining the effects of the bidirectional nutrition-stress interplay in pregnancy on fetal programming of brain development are beginning to emerge in the literature. This review incorporates all currently available animal and human studies of this interplay and provides a synthesis and critical discussion of findings. Nine of the 10 studies included here assessed nutrition-stress interactions and offspring neurodevelopmental or brain development outcomes. Despite significant heterogeneity in study design and methodology, two broad patterns of results emerge to suggest that the effects of prenatal stress on various aspects of brain development may be mitigated by 1) higher fat diets or increased intake and/or status of specific dietary fats and 2) higher dietary intake or supplementation of targeted nutrients. The limitations of these studies are discussed, and recommendations are provided for future research to expand on this important area of fetal programming of brain development.

Published
2019

181. Maternal Cortisol Concentrations During Pregnancy and Sex-Specific Associations With Neonatal Amygdala Connectivity and Emerging Internalizing Behaviors.

Author

Graham, Alice M, Graham, Alice M, Rasmussen, Jerod M, Entringer, Sonja, Ben Ward, Elizabeth, Rudolph, Marc D, Gilmore, John H, Styner, Martin, Wadhwa, Pathik D, Fair, Damien A, Buss, Claudia, Graham, Alice M, Graham, Alice M, Rasmussen, Jerod M, Entringer, Sonja, Ben Ward, Elizabeth, Rudolph, Marc D, Gilmore, John H, Styner, Martin, Wadhwa, Pathik D, Fair, Damien A, and Buss, Claudia

Abstract

BACKGROUND:Maternal cortisol during pregnancy has the potential to influence rapidly developing fetal brain systems that are commonly altered in neurodevelopmental and psychiatric disorders. Research examining maternal cortisol concentrations across pregnancy and offspring neurodevelopment proximal to birth is needed to advance understanding in this area and lead to insight into the etiology of these disorders. METHODS:Participants were 70 adult women recruited during early pregnancy and their infants born after 34 weeks gestation. Maternal cortisol concentrations were assessed serially over 4 days in early, mid, and late gestation. Resting state functional connectivity magnetic resonance imaging of the neonatal amygdala was examined. Mothers reported on children's internalizing behavior problems at 24 months of age. RESULTS:Maternal cortisol concentrations during pregnancy were significantly associated with neonatal amygdala connectivity in a sex-specific manner. Elevated maternal cortisol was associated with stronger amygdala connectivity to brain regions involved in sensory processing and integration, as well as the default mode network in girls, and with weaker connectivity to these brain regions in boys. Elevated maternal cortisol was associated with higher internalizing symptoms in girls only, and this association was mediated by stronger neonatal amygdala connectivity. CONCLUSIONS:Normative variation in maternal cortisol during pregnancy is associated with the coordinated functioning of the amygdala soon after birth in a sex-specific manner. The identified pathway from maternal cortisol to higher internalizing symptoms in girls via alterations in neonatal amygdala connectivity may be relevant for the etiology of sex differences in internalizing psychiatric disorders, which are more prevalent in women.

Published
2019

182. Newborn amygdala connectivity and early emerging fear.

Author

Thomas, Elina, Thomas, Elina, Buss, Claudia, Rasmussen, Jerod M, Entringer, Sonja, Ramirez, Julian SB, Marr, Mollie, Rudolph, Marc D, Gilmore, John H, Styner, Martin, Wadhwa, Pathik D, Fair, Damien A, Graham, Alice M, Thomas, Elina, Thomas, Elina, Buss, Claudia, Rasmussen, Jerod M, Entringer, Sonja, Ramirez, Julian SB, Marr, Mollie, Rudolph, Marc D, Gilmore, John H, Styner, Martin, Wadhwa, Pathik D, Fair, Damien A, and Graham, Alice M

Abstract

Connectivity between the amygdala, insula (Amygdala-aI) and ventral medial prefrontal cortex (Amygdala-vmPFC) have been implicated in individual variability in fear and vulnerability to psychiatric disorders. However, it is currently unknown to what extent connectivity between these regions in the newborn period is relevant for the development of fear and other aspects of negative emotionality (NE), such as sadness. Here, we investigate newborn Am-Ins and Am-vmPFC resting state functional connectivity in relation to developmental trajectories of fear and sadness over the first two years of life using data from the Infant Behavior Questionnaire Revised (IBQ-R) and Early Childhood Behavior Questionnaire (ECBQ) (N=62). Stronger newborn amygdala connectivity predicts higher fear and sadness at 6-months-of-age and less change from 6 to 24-months-of-age. Interestingly, Am-Ins connectivity was specifically relevant for fear and not sadness, while Am-vmPFC was associated only with sadness. Associations remained consistent after considering variation in maternal sensitivity and maternal postnatal depressive symptomology. Already by the time of birth, individual differences in amygdala connectivity are relevant for the expression of fear over the first two-years-of-life. Additionally, specificity is observed, such that connections relevant for fear development are distinct from those predicting sadness trajectories.

Published
2019

183. Stress and immunosenescence: The role of telomerase.

Author

de Punder, Karin, de Punder, Karin, Heim, Christine, Wadhwa, Pathik D, Entringer, Sonja, de Punder, Karin, de Punder, Karin, Heim, Christine, Wadhwa, Pathik D, and Entringer, Sonja

Abstract

Chronic stress is associated with the accelerated aging of the immune system and represents a potent risk factor for the development and progression of a wide range of physical and mental disorders. The elucidation of molecular pathways and mechanisms underlying the link between stress and cellular aging is an area of considerable interest and investigation. In this context, telomere biology has emerged as a particularly attractive candidate mechanism. Several studies have linked immune cell telomere length with stress-related conditions and states, and also with several physical and mental disorders. Because the cellular reverse transcriptase enzyme telomerase is the primary regulator of telomere length (by adding telomeric DNA to telomeres and thereby attenuating telomere shortening), the understanding of its regulation and regulatory functions constitutes a prime target for developing strategies to prevent, attenuate or reverse the adverse consequences of immune system aging (immunosenescence). In this review we provide an overview of the mechanistic pathways linking telomerase with stress and cellular aging, with an emphasis on the immune system. We summarize and synthesize the current state of the literature on immune cell telomerase in different stress- and aging-related disease states and provide recommendations for future research directions.

Published
2019

184. A Role of Oxytocin Receptor Gene Brain Tissue Expression Quantitative Trait Locus rs237895 in the Intergenerational Transmission of the Effects of Maternal Childhood Maltreatment.

Author

Toepfer, Philipp, Toepfer, Philipp, O'Donnell, Kieran J, Entringer, Sonja, Heim, Christine M, Lin, David TS, MacIsaac, Julia L, Kobor, Michael S, Meaney, Michael J, Provençal, Nadine, Binder, Elisabeth B, Wadhwa, Pathik D, Buss, Claudia, Toepfer, Philipp, Toepfer, Philipp, O'Donnell, Kieran J, Entringer, Sonja, Heim, Christine M, Lin, David TS, MacIsaac, Julia L, Kobor, Michael S, Meaney, Michael J, Provençal, Nadine, Binder, Elisabeth B, Wadhwa, Pathik D, and Buss, Claudia

Abstract

ObjectiveWomen exposed to childhood maltreatment (CM) are more likely to exhibit insensitive parenting, which may have consequences for their offspring's development. Variation in the oxytocin-receptor gene (OXTR) moderates risk of CM-associated long-term sequelae associated with mother-child attachment, although functionality of previously investigated single nucleotide polymorphisms (SNPs) remained elusive. Here, we investigated the role of OXTR rs237895, a brain tissue expression quantitative trait locus (eQTL), as a moderator of the relationship between CM and maternal behavior (MB) and the association between MB and offspring attachment security.MethodOf 110 women with information on rs237895 genotype (T-allele = 64, CC = 46), 107 had information on CM (CTQ) and 99 on standardized observer-based ratings of MB at 6 months postpartum (responsivity and detachment), which were used in principal component analysis to obtain a latent factor representing MB. Offspring (n = 86) attachment was evaluated at 12 months of age. Analyses predicting MB were adjusted for socioeconomic status, age, postpartum depression, and genotype-based ethnicity. Analyses predicting child attachment were adjusted for infant sex, socioeconomic status, and postpartum depression.Resultsrs237895 significantly moderated the relationship between CM and MB (F1;66 = 7.99, p < .01), indicating that CM was associated with maternal insensitivity only in high-OXTR-expressing T-allele carriers but not in low-OXTR-expressing CC homozygotes. Moreover, maternal insensitivity predicted offspring insecure attachment (B = -0.551; p < .05).ConclusionWomen with a high OXTR expressing genotype are more susceptible to CM-related impairments in MB that, in turn, predict attachment security in their children, supporting the role of the OT system in the intergenerational transmission of risk associated with maternal CM.

Published
2019

186. Lifetime Psychosocial Stress Exposure Associated with Hypertensive Disorders of Pregnancy.

Author

Caplan, Madeleine, Keenan-Devlin, Lauren S., Freedman, Alexa, Grobman, William, Wadhwa, Pathik D., Buss, Claudia, Miller, Gregory E., and Borders, Ann E.B.

Subjects
HYPERTENSION risk factors, RESEARCH, INTERLEUKINS, BIOMARKERS, CONFIDENCE intervals, MEDICAL cooperation, EXPERIENCE, SOCIOECONOMIC factors, INTERFERONS, PREGNANCY outcomes, TUMOR necrosis factors, LOGISTIC regression analysis, ODDS ratio, SMOKING, BODY mass index, PSYCHOLOGICAL stress, LONGITUDINAL method, PREGNANCY
Abstract

Objective  Hypertensive disorders of pregnancy (HDP) complicate 5 to 10% of all pregnancies and are a major cause of pregnancy-related morbidity. Exposure to psychosocial stress has been associated with systemic inflammation and adverse birth outcomes in pregnant women. Thus, it is probable that psychosocial stress and inflammation play a role in the development of HDP. The primary objective of this analysis was to determine if a woman's lifetime psychosocial stress exposure was associated with an increased risk of HDP. Additionally, we examined whether serum inflammation was an underlying biological mediator for this relationship. Study Design  A multisite prospective study was conducted in a sociodemographically diverse cohort of 647 pregnant women. At a study visit between 12 and 20 6/7 weeks' gestation, maternal psychosocial stress was assessed with six validated assessments and inflammation was measured via log-transformed serum concentrations of interferon-γ, interleukin (IL)-10, IL-13, IL-6, IL-8, and tumor necrosis factor-α. A composite stress score was calculated for each participant from the six stress assessments. The diagnosis of HDP was abstracted from the medical record and was defined as the presence of gestational hypertension after 20 weeks of pregnancy and/or preeclampsia. The association between composite stress and HDP was determined using binary logistic regression. Inflammation, using the six inflammatory biomarkers, was tested as a potential mediator between stress and HDP. Results  Participants with higher composite stress scores were more likely to develop HDP (odds ratio [OR]: 1.50, 95% confidence interval [CI]: 1.06–2.12). When adjusted for known risk modifiers, including maternal age, race/ethnicity, parity, pre-pregnancy body mass index, diabetes, chronic hypertension, and smoking during pregnancy, the risk remained unchanged (OR: 1.50, 95% CI: 1.03–2.20). No mediation effect by inflammation was observed. Conclusion  Independent of known risk factors, women exposed to greater composite stress burden across the life course are at increased risk of developing HDP. Key Points This study was conducted to determine if women with high levels of psychosocial stress have differences in risk for hypertensive disorders of pregnancy (HDP). Independent of known risk factors, women with increased lifetime psychosocial burden are at higher risk for HDP. A model that captures multiple domains of life stress may better predict HDP than a unimodal stress assessment. [ABSTRACT FROM AUTHOR]

Published
2021
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188. Maternal Inflammation During Pregnancy and Offspring Brain Development: The Role of Mitochondria

Author

Gyllenhammer, Lauren E., Rasmussen, Jerod M., Bertele, Nina, Halbing, Amy, Entringer, Sonja, Wadhwa, Pathik D., and Buss, Claudia

Abstract

The association between maternal immune activation (MIA) during pregnancy and risk for offspring neuropsychiatric disorders has been increasingly recognized over the past several years. Among the mechanistic pathways that have been described through which maternal inflammation during pregnancy may affect fetal brain development, the role of mitochondria has received little attention. In this review, the role of mitochondria as a potential mediator of the association between MIA during pregnancy and offspring brain development and risk for psychiatric disorders will be proposed. As a basis for this postulation, convergent evidence is presented supporting the obligatory role of mitochondria in brain development, the role of mitochondria as mediators and initiators of inflammatory processes, and evidence of mitochondrial dysfunction in preclinical MIA exposure models and human neurodevelopmental disorders. Elucidating the role of mitochondria as a potential mediator of MIA-induced alterations in brain development and neurodevelopmental disease risk may not only provide new insight into the pathophysiology of mental health disorders that have their origins in exposure to infection/immune activation during pregnancy but also offer new therapeutic targets.

Published
2022
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191. Stress during pregnancy and gestational weight gain

Author

Kominiarek, Michelle A, Grobman, William, Adam, Emma, Buss, Claudia, Culhane, Jennifer, Entringer, Sonja, Simhan, Hyagriv, Wadhwa, Pathik D, Kim, Kwang-Youn, Keenan-Devlin, Lauren, and Borders, Ann

Subjects
Psychiatric Status Rating Scales, Adult, Prevention, Clinical Sciences, Gestational Age, Stress, Pediatrics, United States, Gestational Weight Gain, Body Mass Index, Pregnancy Complications, Paediatrics and Reproductive Medicine, Young Adult, Logistic Models, Risk Factors, Pregnancy, Clinical Research, Humans, Psychological, Female, Obesity, Prospective Studies
Abstract

ObjectiveTo evaluate the association between prenatal stress and gestational weight gain (GWG).Study designThis was an analysis of women recruited between 2013-2015 from four sites in the US. We tested associations between responses at 32-35 weeks to the Life Experiences Survey (LES), a 37-item measure of events and perceived stress, and GWG categories. Bivariable comparisons and logistic regression were used to estimate the association between the total LES score and the odds of achieving adequate GWG.ResultAmong the 725 women, those with adequate GWG had lower median LES scores (5) compared to women with inadequate (7) and excessive (7) GWG, p = 0.02. After adjusting for age, initial BMI, income, education, marital status and gestational diabetes, lower LES scores (multiples of the median) were associated with adequate GWG (aOR 0.81, 95% CI 0.67-0.98).ConclusionLower reported stress, as measured by the LES, was associated with a greater chance of women achieving adequate GWG. This relationship highlights the potential for interventions directed toward psychosocial support to have salutary effects upon GWG.

Published
2018

192. Cervicovaginal microbiome composition drives metabolic profiles in healthy pregnancy

Author

Oliver, Andrew, primary, LaMere, Brandon, additional, Weihe, Claudia, additional, Wandro, Stephen, additional, Lindsay, Karen L., additional, Wadhwa, Pathik D., additional, Mills, David A., additional, Pride, David, additional, Fiehn, Oliver, additional, Northen, Trent, additional, de Raad, Markus, additional, Li, Huiying, additional, Martiny, Jennifer B.H., additional, Lynch, Susan, additional, and Whiteson, Katrine, additional

Published
2019
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193. The PedBE clock accurately estimates DNA methylation age in pediatric buccal cells

Author

McEwen, Lisa M., primary, O’Donnell, Kieran J., additional, McGill, Megan G., additional, Edgar, Rachel D., additional, Jones, Meaghan J., additional, MacIsaac, Julia L., additional, Lin, David Tse Shen, additional, Ramadori, Katia, additional, Morin, Alexander, additional, Gladish, Nicole, additional, Garg, Elika, additional, Unternaehrer, Eva, additional, Pokhvisneva, Irina, additional, Karnani, Neerja, additional, Kee, Michelle Z. L., additional, Klengel, Torsten, additional, Adler, Nancy E., additional, Barr, Ronald G., additional, Letourneau, Nicole, additional, Giesbrecht, Gerald F., additional, Reynolds, James N., additional, Czamara, Darina, additional, Armstrong, Jeffrey M., additional, Essex, Marilyn J., additional, de Weerth, Carolina, additional, Beijers, Roseriet, additional, Tollenaar, Marieke S., additional, Bradley, Bekh, additional, Jovanovic, Tanja, additional, Ressler, Kerry J., additional, Steiner, Meir, additional, Entringer, Sonja, additional, Wadhwa, Pathik D., additional, Buss, Claudia, additional, Bush, Nicole R., additional, Binder, Elisabeth B., additional, Boyce, W. Thomas, additional, Meaney, Michael J., additional, Horvath, Steve, additional, and Kobor, Michael S., additional

Published
2019
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195. Positive life events during pregnancy and cellular aging in infants

Author

Lazarides, Claudia, primary, Epel, Elissa S., additional, Lin, Jue, additional, Blackburn, Elizabeth H., additional, Pokhvisneva, Irina, additional, Oldach, Matthew J., additional, Meaney, Michael J., additional, O’Donnell, Kieran J., additional, Kobor, Michael S., additional, MacIsaac, Julie L., additional, Lin, David T., additional, Buss, Claudia, additional, Simhan, Hyagriv N., additional, Wadhwa, Pathik D., additional, and Entringer, Sonja, additional

Published
2019
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197. Maternal prenatal depression and infant DNA methylome maturation: Developmental regulation of DNA methylation and relevance for infant behavior

Author

Toepfer, Philipp, primary, Pokhvisneva, Irina, additional, Garg, Elika, additional, Entringer, Sonja, additional, Heim, Christine M., additional, Kobor, Michael S., additional, Provencal, Nadine, additional, Binder, Elisabeth B., additional, Wadhwa, Pathik D., additional, Meaney, Michael J., additional, Buss, Claudia, additional, and ÓDonnell, Kieran J., additional

Published
2019
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199. Newborn amygdala connectivity and early emerging fear

Author

Thomas, Elina, primary, Buss, Claudia, additional, Rasmussen, Jerod M., additional, Entringer, Sonja, additional, Ramirez, Julian S.B., additional, Marr, Mollie, additional, Rudolph, Marc D., additional, Gilmore, John H., additional, Styner, Martin, additional, Wadhwa, Pathik D., additional, Fair, Damien A., additional, and Graham, Alice M., additional

Published
2019
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200. Dynamic DNA methylation changes in the maternal oxytocin gene locus (OXT) during pregnancy predict postpartum maternal intrusiveness

Author

Toepfer, Philipp, primary, O’Donnell, Kieran J., additional, Entringer, Sonja, additional, Garg, Elika, additional, Heim, Christine M., additional, Lin, David T.S., additional, MacIsaac, Julia L., additional, Kobor, Michael S., additional, Meaney, Michael J., additional, Provençal, Nadine, additional, Binder, Elisabeth B., additional, Wadhwa, Pathik D., additional, and Buss, Claudia, additional

Published
2019
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