首页> 美国卫生研究院文献>Journal of the Endocrine Society >SAT-715 Bisphenol-A Alters Pancreatic B-Cell Proliferation and Mass in an Estrogen Receptor Beta-Dependent Manner
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SAT-715 Bisphenol-A Alters Pancreatic B-Cell Proliferation and Mass in an Estrogen Receptor Beta-Dependent Manner

机译:SAT-715双酚-A在雌激素受体β依赖性方式中改变胰腺B细胞增殖和质量

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摘要

Bisphenol-A (BPA) is one of the highest volume chemicals produced worldwide. It is used as the base compound in the manufacture of polycarbonate plastics, epoxies and resins. Humans are consistently exposed to BPA and consistently it has been detected in the majority of individuals examined. Experimental research in animals, as well as human epidemiological studies, converge to conclude that BPA is a risk factor for the development of type 2 diabetes. In previous studies we have demonstrated that the exposure to BPA during embryonic development promote an increment of pancreatic β-cell mass. This was correlated with increased β-cell division and altered global gene expression in pancreatic β-cells. The aim of this work was to determinate whether ERβ was involved in the in the β-cell mass and proliferation increment observed in male mice offspring. ERβ+/- pregnant mice were treated with vehicle or BPA (10 μg/kg/day) from day 9 to 16 of gestation. Offspring pancreatic β-cell mass was measured at postnatal day 0 (P0) and 30 (P30). For ex vivo experiments Wild-type (WT) and ERβ-/- neonates as well as adult male and female mice were used. For in vitro, single islets cells were cultured for 48 h in the presence of 10 μmol/L BrdU, and vehicle, BPA (1, 10, 100 nM) or the specific ERβ agonist WAY200070 (1, 10, 100 nM). β-cell proliferation rate was quantified as the percentage of BrdU-positive pancreatic β-cells. In vivo exposure to BPA during pregnancy promoted an increment of pancreatic β-cell mass and proliferation in WT mice at P30 which was absent in ERβ -/- mice. In order to explore if these changes were related to a direct action of BPA on pancreatic β-cell division we performed a series of ex vivo experiments. Augmented β-cell proliferation rate was observed in BPA-exposed β-cells isolated from both adult male and female WT animals in comparison to controls. The increment was significant at all BPA doses tested. The effect was imitated by the selective ERβ agonist, WAY200070, and was abolished in cells from ERβ-/- mice. We also explored the effects of BPA in pancreatic β-cells from neonates and found an increment in BPA-exposed cells compared to controls, although the difference was only significant at the dose of 1 nM. A similar effect was observed in neonate cells treated with WAY200070 (10 nM). The effects on β-cell replication were abolished in cells from ERβ-/- neonate mice treated either with BPA or WAY200070. Our findings suggest that BPA modulate pancreatic β-cell growth and mass in an ERβ-dependent manner. This could have important implications for metabolic programming of T2DM. Ministerio de Economía y Competitividad, Agencia Estatal de Investigación (AEI) and Fondo Europeo de Desarrollo Regional (FEDER) grants BPU2017-86579-R (AN) and BFU2016-77125-R (IQ); Generalitat Valenciana PROMETEO II/2015/016 (AN). CIBERDEM is an initiative of the Instituto de Salud Carlos III.
机译:双酚-A(BPA)是全球生产的最高体积化学品之一。它用作制造聚碳酸酯塑料,环氧树脂和树脂中的基础化合物。人类始终如一地暴露于BPA,并且一致地在检查的大多数人中被检测到。动物的实验研究以及人体流行病学研究,结合得出结论,BPA是2型糖尿病患者的危险因素。在先前的研究中,我们已经证明,在胚胎发育期间暴露于BPA促进胰腺β细胞质量的增量。这与胰腺β细胞中的β细胞分裂增加和改变的全局基因表达相关。这项工作的目的是测定ERβ是否参与在雄性小鼠后代中观察到的β细胞质量和增殖增量。将ERβ+/-怀孕的小鼠从妊娠的第9天与载体或BPA(10μg/ kg /天)处理。在后期0(p0)和30(p30)下测量后代胰腺β细胞质量。对于前体内实验,使用野生型(WT)和Erβ/ - 新生儿以及成年男性和雌性小鼠。对于体外,在10μmol/ L Brdu的存在下培养单个胰岛细胞48小时,并且载体,BPA(1,10,100nm)或特定的ERβ激动剂Way200070(1,10,100nm)。量化β-细胞增殖率为Brdu阳性胰腺β细胞的百分比。在妊娠期间,体内暴露于BPA促进了在ERβ/ - 小鼠中不存在的P30的胰腺β细胞质量和增殖中的增量。为了探讨这些变化与BPA对胰腺β-细胞分裂的直接作用有关,我们进行了一系列的离体实验。与对照相比,在从成年男性和雌性WT动物中分离的BPA暴露的β细胞中观察到增强β细胞增殖率。在所有BPA剂量测试中,增量是显着的。通过选择性ERβ激动剂,Way200070仿效果,并在Erβ/ - 小鼠中消除了细胞。我们还探讨了BPA在新生儿的胰腺β细胞中的影响,并与对照相比,BPA暴露细胞中的增量,尽管差异在1nm的剂量下仅显着。在用Way200070(10nm)处理的新生儿细胞中观察到类似的效果。用BPA或Way200070治疗的Erβ/ - 新生大鼠的细胞中对β细胞复制的影响被废除。我们的研究结果表明,BPA以ERβ依赖性方式调节胰腺β细胞生长和质量。这可能对T2DM的代谢编程具有重要意义。部:EconomíaÿCompetitividad,AGENCIA Estatal德Investigación(AEI)和丰多欧洲人德DESARROLLO区域(FEDER)授予BPU2017-86579-R(AN)和BFU2016-77125-R(IQ); Generalit at Valenciana Prometeo II / 2015/016(AN)。 Ciberdem是Instituto de Salud Carlos III的倡议。

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