Developmental programming: Interaction between prenatal BPA and postnatal overfeeding on cardiac tissue gene expression in female sheep

Koneva, Lada A.; Vyas, Arpita; McEachin, Richard C.; Puttabyatappa, Muraly; Wang, H.‐S.; Sartor, Maureen A.; Padmanabhan, Vasantha

doi:10.1002/em.22071

Cited by 11 publications

(9 citation statements)

References 93 publications

(123 reference statements)

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“…As opposed to lack of effect of prenatal BPA on fetal male liver, prenatal BPA treatment increased the heart/body weight ratio at GD90 in males, alone. Consistent with the lack of effect on the female heart during fetal life, there were no effects of prenatal BPA treatment on blood pressure or morphometric measures in adult BPA‐treated offspring (Koneva et al, ; MohanKumar et al, ). However, prenatal BPA treatment upregulated several genes involved in the regulation of myocardium growth, heart development and remodeling, and the downregulation of genes involved in cellular respiration and inflammation in adult prenatal BPA‐treated females (Koneva et al, ).…”

Section: Discussionmentioning

confidence: 77%

“…Consistent with the lack of effect on the female heart during fetal life, there were no effects of prenatal BPA treatment on blood pressure or morphometric measures in adult BPA‐treated offspring (Koneva et al, ; MohanKumar et al, ). However, prenatal BPA treatment upregulated several genes involved in the regulation of myocardium growth, heart development and remodeling, and the downregulation of genes involved in cellular respiration and inflammation in adult prenatal BPA‐treated females (Koneva et al, ). Prenatal BPA treatment was also found to reduce collagen expression in the right ventricle (MohanKumar et al, ).…”

Section: Discussionmentioning

confidence: 77%

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Developmental programming: Sex‐specific programming of growth upon prenatal bisphenol A exposure

Vyas

Veiga-López

et al. 2019

J of Applied Toxicology

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In both human and animals, in utero exposure to bisphenol A (BPA), an endocrine‐disrupting chemical used in the production of plastics and epoxy resins, has been shown to affect offspring reproductive and metabolic health during adult life. We hypothesized that the effect of prenatal exposure to environmentally relevant doses of BPA will be evident during fetal organogenesis and fetal/postnatal growth trajectory. Pregnant ewes were administered BPA subcutaneously from 30 to 90 days of gestation (term 147 days). Fetal organ weight, anthropometric measures, maternal/fetal hormones and postnatal growth trajectory were measured in both sexes. Gestational BPA administration resulted in higher accumulation in male than female fetuses only at fetal day 65, with minimal impact on fetal/maternal steroid milieu in both sexes at both time points. BPA‐treated male fetuses were heavier than BPA‐treated female fetuses at fetal day 90 whereas this sex difference was not evident in the control group. At the organ level, liver weight was reduced in prenatal BPA‐treated female fetuses, while heart and thyroid gland weights were increased in BPA‐treated male fetuses relative to their sex‐matched control groups. Prenatal BPA treatment also altered the postnatal growth trajectory in a sex‐specific manner. Males grew slower during the early postnatal period and caught up later. Females, in contrast, demonstrated the opposite growth trend. Prenatal BPA‐induced changes in fetal organ differentiation and early life growth strongly implicate translational relevance of in utero contributions to reproductive and metabolic defects previously reported in adult female offspring.

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Section: Discussionmentioning

confidence: 77%

Section: Discussionmentioning

confidence: 77%

Developmental programming: Sex‐specific programming of growth upon prenatal bisphenol A exposure

Vyas

Veiga-López

et al. 2019

J of Applied Toxicology

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“…Importantly, previous studies have demonstrated that the postnatal environment could amplify the final phenotypic outcomes programmed by early developmental insults [27][28][29]. Nonetheless, to the best of our knowledge, no studies have reported on the responsiveness of intestinal function to postnatal insults, ensuing the metabolic disruptions programmed by prenatal BPA exposure.…”

Section: Introductionmentioning

confidence: 93%

Prenatal Bisphenol a Exposure and Postnatal Trans Fat Diet Alter Small Intestinal Morphology and Its Global DNA Methylation in Male Sprague-Dawley Rats, Leading to Obesity Development

et al. 2022

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In this study, we aimed to determine whether a postnatal trans fat diet (TFD) could aggravate prenatal bisphenol A (BPA) exposure effects on offspring’s small intestine and adulthood obesity, due to the relatively sparse findings on how the interaction between these two variables interrupt the small intestinal cells. Twelve pregnant rats were administered with either unspiked drinking water (control; CTL) or BPA-spiked drinking water throughout pregnancy. Twelve weaned pups from each pregnancy group were then given either a normal diet (ND) or TFD from postnatal week (PNW) 3 until PNW14, divided into control offspring on normal diet (CTL-ND), BPA-exposed offspring on normal diet (BPA-ND), control offspring on trans fat diet (CTL-TFD), and BPA offspring on trans fat diet (BPA-TFD) groups. Body weight (BW), waist circumference, and food and water intake were measured weekly in offspring. At PNW14, small intestines were collected for global DNA methylation and histological analyses. Marked differences in BW were observed starting at PNW9 in BPA-TFD (389.5 ± 10.0 g; p < 0.05) relative to CTL-ND (339.0 ± 7.2 g), which persisted until PNW13 (505.0 ± 15.6 g). In contrast, water and food intake between offspring were significantly different (p < 0.01–0.05) at earlier ages only (PNW4–6 and PNW7–9, respectively). Furthermore, substantial differences in the general parameters of the intestinal structures were exclusive to ileum crypt length alone, whereby both BPA-ND (150.5 ± 5.1 μm; p < 0.001), and BPA-TFD (130.3 ± 9.9 μm; p < 0.05) were significantly longer than CTL-ND (96.8 ± 8.9 μm). Moreover, BPA-ND (2.898 ± 0.147%; p < 0.05) demonstrated global small intestinal hypermethylation when compared to CTL-ND and CTL-TFD (1.973 ± 0.232% and 1.913 ± 0.256%, respectively). Prenatal BPA exposure may significantly affect offspring’s physiological parameters and intestinal function. Additionally, our data suggest that there might be compensatory responses to postnatal TFD in the combined BPA prenatal group (BPA-TFD).

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“…Maternal hyperglycemia in pregnancy is independently associated with the offspring’s risk for glucose intolerance, obesity and an increase in blood pressure in seven-year-old children, with only girls being obese [ 51 ]. In female sheep, after prenatal bisphenol A (BPA, commonly found in polycarbonate plastic and epoxy resins) exposure, postnatal overfeeding/adiposity, and the combination, led to myocardial transcriptional changes, and despite different gene profiles, still influenced similar signaling pathways [ 21 ]. Genes altered by the programming insult were implicated in obesity, hypertension or heart disease [ 21 ].…”

Section: High Fat Programming: Sex-specificity Altered Cardiac Gementioning

confidence: 99%

“…In female sheep, after prenatal bisphenol A (BPA, commonly found in polycarbonate plastic and epoxy resins) exposure, postnatal overfeeding/adiposity, and the combination, led to myocardial transcriptional changes, and despite different gene profiles, still influenced similar signaling pathways [ 21 ]. Genes altered by the programming insult were implicated in obesity, hypertension or heart disease [ 21 ]. In rats, a maternal HFD causes cardiac hypertrophy; increases cardiac susceptibility to ischemic-reperfusion injury only in adult male offspring, and differentially regulates cardiac angiotensin II (AngII) receptor type 1 (AGTR1) and type 2 (AGTR2) expression [ 48 ].…”

Section: High Fat Programming: Sex-specificity Altered Cardiac Gementioning

confidence: 99%

High Fat Programming and Cardiovascular Disease

Cerf

2018

Medicina

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Programming is triggered through events during critical developmental phases that alter offspring health outcomes. High fat programming is defined as the maintenance on a high fat diet during fetal and/or early postnatal life that induces metabolic and physiological alterations that compromise health. The maternal nutritional status, including the dietary fatty acid composition, during gestation and/or lactation, are key determinants of fetal and postnatal development. A maternal high fat diet and obesity during gestation compromises the maternal metabolic state and, through high fat programming, presents an unfavorable intrauterine milieu for fetal growth and development thereby conferring adverse cardiac outcomes to offspring. Stressors on the heart, such as a maternal high fat diet and obesity, alter the expression of cardiac-specific factors that alter cardiac structure and function. The proper nutritional balance, including the fatty acid balance, particularly during developmental windows, are critical for maintaining cardiac structure, preserving cardiac function and enhancing the cardiac response to metabolic challenges.

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Developmental programming: Interaction between prenatal BPA and postnatal overfeeding on cardiac tissue gene expression in female sheep

Cited by 11 publications

References 93 publications

Developmental programming: Sex‐specific programming of growth upon prenatal bisphenol A exposure

Developmental programming: Sex‐specific programming of growth upon prenatal bisphenol A exposure

Prenatal Bisphenol a Exposure and Postnatal Trans Fat Diet Alter Small Intestinal Morphology and Its Global DNA Methylation in Male Sprague-Dawley Rats, Leading to Obesity Development

High Fat Programming and Cardiovascular Disease

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