Transmaternal Bisphenol A Exposure Accelerates Diabetes Type 1 Development in NOD Mice

Bodin, Johanna; Bølling, Anette Kocbach; Becher, Rune; Kuper, C. Frieke; Løvik, Martinus; Nygaard, Unni Cecilie

doi:10.1093/toxsci/kft242

Cited by 89 publications

(69 citation statements)

References 71 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In a rat model, females exposed to the phthalate DEHP throughout gestation and perinatal development exhibited hyperglycemia in the presence of reduced insulin levels [504]. Histological evaluation of pancreatic islets from weanlings revealed reductions in β-cell mass, reduced islet insulin content, and disruptions in β-cell ultrastructure [491].…”

Section: Mdcs and Metabolism-relevant Diseasesmentioning

confidence: 99%

“…Similarly, rats exposed to DEHP throughout gestation and perinatal development exhibited hyperglycemia in the presence of reduced insulin levels [504] along with reductions in β-cell mass, reduced islet insulin content, and disruptions in β-cell ultrastructure [491]. Sex-specific effects of DEHP on measures of insulin resistance have been reported in some epidemiological studies[495].…”

Section: Mdcs and Metabolism-relevant Diseasesmentioning

confidence: 99%

See 1 more Smart Citation

Metabolism disrupting chemicals and metabolic disorders

Heindel

Blumberg

Cave

et al. 2017

Reproductive Toxicology

814

651

View full text Add to dashboard Cite

The recent epidemics of metabolic diseases, obesity, type 2 diabetes(T2D), liver lipid disorders and metabolic syndrome have largely been attributed to genetic background and changes in diet, exercise and aging. However, there is now considerable evidence that other environmental factors may contribute to the rapid increase in the incidence of these metabolic diseases. This review will examine changes to the incidence of obesity, T2D and non-alcoholic fatty liver disease (NAFLD), the contribution of genetics to these disorders and describe the role of the endocrine system in these metabolic disorders. It will then specifically focus on the role of endocrine disrupting chemicals (EDCs) in the etiology of obesity, T2D and NAFLD while finally integrating the information on EDCs on multiple metabolic disorders that could lead to metabolic syndrome. We will specifically examine evidence linking EDC exposures during critical periods of development with metabolic diseases that manifest later in life and across generations.

show abstract

Section: Mdcs and Metabolism-relevant Diseasesmentioning

confidence: 99%

Section: Mdcs and Metabolism-relevant Diseasesmentioning

confidence: 99%

Metabolism disrupting chemicals and metabolic disorders

Heindel

Blumberg

Cave

et al. 2017

Reproductive Toxicology

814

651

View full text Add to dashboard Cite

show abstract

“…In a different study, gestational and lactational exposure to BPA failed to exacerbate adult EAE [38]. Diabetic (NOD) mice given BPA during gestation generated female offspring with an increased incidence of diabetes [39]. Perinatal BPA exposure accelerated inflammation in a mouse model of virally-induced multiple sclerosis [40].…”

Section: Bisphenol Amentioning

confidence: 99%

“…In NOD mice, BPA exposure increased the number of T REGS , while also increasing production of IL-17 [39]. Thus, BPA-mediated DNA methylation events may play a role in effector cell generation since differentiation of naïve CD4 Tcells into these subsets is regulated in part by DNA methylation.…”

Section: Bisphenol Amentioning

confidence: 99%

Epigenetic underpinnings of developmental immunotoxicity and autoimmune disease

Blossom

Gilbert

2018

Current Opinion in Toxicology

View full text Add to dashboard Cite

The concordance rate for developing autoimmune disease in identical twins is around 50% demonstrating that gene and environmental interactions contribute to disease etiology. The environmental contribution to autoimmune disease is a wide-ranging concept including exposure to immunotoxic environmental chemicals. Because the immune system is immature during development suggests that adult-onset autoimmunity may originate when the immune system is particularly sensitive. Among the pollutants most closely associated with inflammation and/or autoimmunity include Bisphenol-A, mercury, TCDD, and trichloroethylene. These toxicants have been shown to impart epigenetic changes (e.g., DNA methylation) that may alter immune function and promote autoreactivity. Here we review these autoimmune-promoting toxicants and their relation to immune cell epigenetics both in terms of adult and developmental exposure.

show abstract

“…Chronic exposure to BPA accelerated spontaneous insulinitis in non-obese diabetic (NOD) mice, a model of immune-mediated diabetes [39]. In addition, NOD mice exposed to BPA in utero exhibited more severe insulinitis at 11 weeks of age and increased diabetes prevalence at 20 weeks [40•], suggesting that BPA may also play a role in accelerating the decline of β-cell reserve by promoting immune disruption of pancreatic islets, implicating MDCs as possible contributors to increasing T1DM prevalence.…”

Section: Endoplasmic Reticulum and Oxidative Stress In MDC Actionmentioning

confidence: 99%

Polluted Pathways: Mechanisms of Metabolic Disruption by Endocrine Disrupting Chemicals

Mimoto

Nadal

Sargis

2017

Curr Envir Health Rpt

View full text Add to dashboard Cite

Purpose of review Environmental toxicants are increasingly implicated in the global decline in metabolic health. Focusing on diabetes, herein the molecular and cellular mechanisms by which metabolism disrupting chemicals (MDCs) impair energy homeostasis are discussed. Recent findings Emerging data implicate MDC perturbations in a variety of pathways as contributors to metabolic disease pathogenesis, with effects in diverse tissues regulating fuel utilization. Potentiation of traditional metabolic risk factors, such as caloric excess, and emerging threats to metabolism, such as disruptions in circadian rhythms, are important areas of current and future MDC research. Increasing evidence also implicates deleterious effects of MDCs on metabolic programming that occur during vulnerable developmental windows, such as in utero and early post-natal life as well as pregnancy. Summary Recent insights into the mechanisms by which MDCs alter energy homeostasis will advance the field’s ability to predict interactions with classical metabolic disease risk factors and empower studies utilizing targeted therapeutics to treat MDC-mediated diabetes.

show abstract

Transmaternal Bisphenol A Exposure Accelerates Diabetes Type 1 Development in NOD Mice

Cited by 89 publications

References 71 publications

Metabolism disrupting chemicals and metabolic disorders

Metabolism disrupting chemicals and metabolic disorders

Epigenetic underpinnings of developmental immunotoxicity and autoimmune disease

Polluted Pathways: Mechanisms of Metabolic Disruption by Endocrine Disrupting Chemicals

Contact Info

Product

Resources

About