Brainstem expression of SLC6A4, HTR2C, NGF, BDNF, TRKANGF, TRKBBDNF and P75NTR following paternal alcohol exposure in the male mouse

G. Ferraguti, C. Codazzo, C. Petrella, R. Coccurello, M. Ceccanti, M. Fiore
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引用次数: 3

Abstract

We previously showed in the mouse that paternal preconception alcohol exposure (PPAE) affects alcohol sensitivity by analyzing postnatal alcohol preference in the offspring. In this mouse study by using the same animals of the previous investigation we aimed at examining whether or not PPAE may disrupt the epigenetic regulation of postnatal alcohol sensitivity in the offspring by investigating pathways regulating mood, emotion, serotonergic tone and neurotrophins such as nerve growth factor (NGF) and brain-derived neurotrophic factor (BDNF). We analyzed the brainstem gene expression of serotonin transporter Solute Carrier Family 6 Member4 (SLC6A4), 5-Hydroxytryptamine Receptor 2C (HTR2C) binding the neurotransmitter serotonin, and NGF, BDNF and their tropomyosin receptor kinase A (TrkA NGF ) and B (TrKB BDNF ) (high-affinity NGF and BDNF receptors) and p75 NTR (low-affinity, pan-neurotrophins receptor) in adult offspring that underwent or not postnatal alcohol exposure. We found SLC6A4 elevation and decreased HTR2C in the offspring of chronic alcohol-exposed sires. We also disclosed p75 NTR elevation in the offspring of chronically exposed sires as well as postnatal sensitization to low alcohol doses in the offspring of chronically exposed sires for both TrKB BDNF and BDNF. In our PPAE mouse model, where genotype effects can be carefully measured, we observed that the sires’ exposure to alcohol before mating might disrupt the sensitivity to the serotonergic/neurotrophic-associated effects of alcohol influencing the postnatal alcohol preference in the offspring. Biomed Rev 2020; 31: 75-89
雄性小鼠在父亲酒精暴露后脑干SLC6A4、HTR2C、NGF、BDNF、TRKANGF、TRKBBDNF和P75NTR的表达
我们之前通过分析后代出生后的酒精偏好,在小鼠中发现父亲孕前酒精暴露(PPAE)会影响酒精敏感性。在这项小鼠研究中,我们通过研究调节情绪、情绪、血清素能张力和神经营养因子(如神经生长因子(NGF)和脑源性神经营养因子(BDNF)的途径,研究PPAE是否会破坏后代出生后酒精敏感性的表观遗传调节。我们分析了5-羟色胺转运体溶质载体家族6成员4 (SLC6A4)、结合神经递质5-羟色胺受体2C (HTR2C)、NGF、BDNF及其原肌球蛋白受体激酶A (TrkA NGF)和B (TrKB BDNF)(高亲和力NGF和BDNF受体)和p75 NTR(低亲和力泛神经营养因子受体)在出生后酒精暴露或未暴露的成年后代的脑干基因表达。我们发现慢性酒精暴露的后代SLC6A4升高,HTR2C降低。我们还发现,长期暴露的后代中p75 NTR升高,以及长期暴露的后代对低酒精剂量的TrKB BDNF和BDNF的产后致敏。在我们的PPAE小鼠模型中,基因型效应可以被仔细测量,我们观察到雌性在交配前接触酒精可能会破坏对酒精影响后代出生后酒精偏好的血清素能/神经营养相关效应的敏感性。Biomed Rev 2020;31日:75 - 89
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