Differential Effects of 3rd Trimester-Equivalent Binge Ethanol and Tobacco-Specific Nitrosamine Ketone Exposures on Brain Insulin Signaling in Adolescence.

Journal of diabetes and related disorders Pub Date : 2016-01-01 Epub Date: 2016-02-26

Tomas Andreani, Ming Tong, Fusun Gundogan, Elizabeth Silbermann, Suzanne M de la Monte

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Abstract

Background: Fetal alcohol spectrum disorder (FASD) is associated with impairments in insulin and insulin-like growth factor (IGF) signaling through Akt pathways and altered expression of neuro-glial proteins needed for structural and functional integrity of the brain. However, alcohol abuse correlates with smoking, and tobacco smoke contains 4-(methylnitrosamino)-1-(3-pyridyl)-1-butanone (NNK), which like other nitrosamines, impairs insulin and IGF signaling.

Hypothesis: NNK exposure can serve as a co-factor in mediating long-term neuro-developmental abnormalities associated with FASD.

Design: Long Evans rat pups were IP administered ethanol (2 g/kg) on postnatal days (P) 2, 4, 6 and/or NNK (2 mg/kg) on P3, P5, and P7, simulating third trimester human exposures. Temporal lobes from P30 rats (young adolescent) were used to measure signaling through the insulin/IGF-1/Akt pathways by multiplex ELISAs, and expression of neuroglial proteins by duplex ELISAs.

Results: Ethanol, NNK, and ethanol + NNK exposures significantly inhibited insulin receptor tyrosine phosphorylation, and IRS-1 and myelin-associated glycoprotein expression. However, the major long-term adverse effects on Akt pathway downstream signaling and its targeted proteins including choline acetyltransferase, Tau, pTau, ubiquitin, and aspartate-β-hydroxylase were due to NNK rather than ethanol.

Conclusion: Alcohol and tobacco exposures can both contribute to long-term brain abnormalities currently regarded fetal ethanol effects. However, the findings suggest that many of the adverse effects on brain function are attributable to smoking, including impairments in signaling through survival and metabolic pathways, and altered expression of genes that regulate myelin synthesis, maturation and integrity and synaptic plasticity. Therefore, public health measures should address both substances of abuse to prevent "FASD".

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青春期暴露于第三孕期等量狂饮乙醇和烟草特异性亚硝胺酮对脑胰岛素信号的不同影响

背景：胎儿酒精谱系障碍（FASD）与通过 Akt 通路传递胰岛素和胰岛素样生长因子（IGF）信号的损伤以及大脑结构和功能完整性所需的神经胶质蛋白表达的改变有关。然而，酗酒与吸烟有关，而烟草烟雾中含有 4-（甲基亚硝基氨基）-1-（3-吡啶基）-1-丁酮（NNK），它与其他亚硝胺一样，会损害胰岛素和 IGF 信号传导：假设：NNK 暴露可作为介导与 FASD 相关的长期神经发育异常的辅助因子：设计：在出生后第 2、4、6 天和/或第 3、5 和 7 天给 Long Evans 大鼠幼崽 IP 注射乙醇（2 克/千克）和/或 NNK（2 毫克/千克），模拟人类出生后三个月的暴露情况。利用 P30 大鼠（青少年）的颞叶，通过多重 ELISAs 检测胰岛素/IGF-1/Akt 通路的信号传导，并通过双重 ELISAs 检测神经胶质蛋白的表达：结果：暴露于乙醇、NNK 和乙醇 + NNK 会显著抑制胰岛素受体酪氨酸磷酸化以及 IRS-1 和髓鞘相关糖蛋白的表达。然而，NNK而非乙醇对Akt通路下游信号转导及其靶蛋白（包括胆碱乙酰转移酶、Tau、pTau、泛素和天冬氨酸-β-羟化酶）的主要长期不利影响：结论：酒精和烟草接触都会导致长期的大脑异常，目前认为是胎儿乙醇效应。然而，研究结果表明，对大脑功能的许多不利影响都可归因于吸烟，包括通过生存和代谢途径传递信号的障碍，以及调节髓鞘合成、成熟和完整性以及突触可塑性的基因表达的改变。因此，公共卫生措施应针对这两种滥用物质，以预防 "FASD"。

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