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Review
. 2015 Jun 12;13(2):1559325815590395.
doi: 10.1177/1559325815590395. eCollection 2015 Apr-Jun.

Prenatal Exposure to BPA and Offspring Outcomes: The Diabesogenic Behavior of BPA

Paloma Alonso-Magdalena  1 Iván Quesada  2 Ángel Nadal  3
Affiliations
Review

Prenatal Exposure to BPA and Offspring Outcomes: The Diabesogenic Behavior of BPA

Paloma Alonso-Magdalena et al. Dose Response. .

Abstract

Obesity and type 2 diabetes mellitus (T2DM) are the most common metabolic disorders, with prevalence rates that are reaching epidemic proportions. Both are complex conditions affecting virtually all ages and with serious health consequences. The underlying cause of the problem is still puzzling, but both genetic and environmental factors including unhealthy diet, sedentary lifestyle, or the exposure to some environmental endocrine disrupting chemicals (EDCs) are thought to have a causal influence. In addition, the impact of early environment has recently emerged as an important factor responsible for the increased propensity to develop adult-onset metabolic disease. Suboptimal maternal nutrition during critical windows in fetal development is the most commonly studied factor affecting early programming of obesity and T2DM. In recent years, increasing experimental evidence shows that exposure to EDCs could also account for this phenomenon. In the present review, we will overview the most relevant findings that confirm the critical role of bisphenol-A, one of the most widespread EDCs, in the development of metabolic disorders.

Keywords: bisphenol-A; diabetes; metabolic disorders; obesity.

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References

    1. Alonso-Magdalena P, Laribi O, Ropero AB, Fuentes E, Ripoll C, Soria B, Nadal A. (2005). Low doses of bisphenol A and diethylstilbestrol impair Ca2+ signals in pancreatic alpha-cells through a nonclassical membrane estrogen receptor within intact islets of Langerhans. Environ Health Perspect 113, 969–977. - PMC - PubMed
    1. Alonso-Magdalena P, Morimoto S, Ripoll C, Fuentes E, Nadal A. (2006). The estrogenic effect of bisphenol A disrupts pancreatic beta-cell function in vivo and induces insulin resistance. Environ Health Perspect 114, 106–112. - PMC - PubMed
    1. Alonso-Magdalena P, Quesada I, Nadal A. (2011). Endocrine disruptors in the etiology of type 2 diabetes mellitus. Nat Rev Endocrinol 7, 346–353. - PubMed
    1. Alonso-Magdalena P, Ropero AB, Carrera MP, Cederroth CR, Baquie M, Gauthier BR, Nef S, Stefani E, Nadal A. (2008). Pancreatic insulin content regulation by the estrogen receptor ER alpha. PLoS One 3, e2069. - PMC - PubMed
    1. Alonso-Magdalena P, Ropero AB, Soriano S, Garcia-Arevalo M, Ripoll C, Fuentes E, Quesada I, Nadal A. (2012). Bisphenol-A acts as a potent estrogen via non-classical estrogen triggered pathways. Mol Cell Endocrinol 355, 201–207. - PubMed

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