首页> 美国卫生研究院文献>Frontiers in Neurology >Differential Expression of Brain Cannabinoid Receptors between Repeatedly Stressed Males and Females may Play a Role in Age and Gender-Related Difference in Traumatic Brain Injury: Implications from Animal Studies
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Differential Expression of Brain Cannabinoid Receptors between Repeatedly Stressed Males and Females may Play a Role in Age and Gender-Related Difference in Traumatic Brain Injury: Implications from Animal Studies

机译:反复承受压力的男性和女性之间脑大麻素受体的差异表达可能在创伤性脑损伤的年龄和性别相关差异中发挥作用:来自动物研究的意义

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摘要

Inconsistent gender differences in the outcome of TBI have been reported. The mechanism is unknown. In a recent male animal study, repeated stress followed by TBI had synergistic effects on brain gene expression and caused greater behavioral deficits. Because females are more likely to develop anxiety after stress and because anxiety is mediated by cannabinoid receptors (CBRs) (CB1 and CB2), there is a need to compare CB1 and CB2 expression in stressed males and females. CB1 and CB2 mRNA expression was determined in the amygdala, hippocampus, prefrontal cortex (PFC), and hypothalamus of adolescent male and female rats after 3 days of repeated tail-shock stress using qPCR. PFC CB1 and CB2 protein levels were determined using Western blot techniques. Both gender and stress had significant effects on brain CB1 mRNA expression levels. Overall, females showed significantly higher CB1 and CB2 mRNA levels in all brain regions than males (p < 0.01). Repeated stress reduced CB1 mRNA levels in the amygdala, hippocampus, and PFC (p < 0.01, each). A gender × stress interaction was found in CB1 mRNA level in the hippocampus (p < 0.05), hypothalamus (p < 0.01), and PFC (p < 0.01). Within-sex one-way ANOVA analysis showed decreased CB1 mRNA in the hippocampus, hypothalamus, and PFC of stressed females (p < 0.01, each) but increased CB1 mRNA levels in the hypothalamus of stressed males (p < 01). There was a gender and stress interaction in prefrontal CB1 receptor protein levels (p < 0.05), which were decreased in stressed females only (p < 0.05). Prefrontal CB2 protein levels were decreased in both male and female animals after repeated stress (p < 0.05, each). High basal levels of CBR expression in young naïve females could protect against TBI damage whereas stress-induced CBR deficits could predict a poor outcome of TBI in repeatedly stressed females. Further animal studies could help evaluate this possibility.
机译:据报道,在TBI结果中性别差异不一致。机制未知。在最近的一项雄性动物研究中,反复施加压力和TBI对大脑基因表达具有协同作用,并导致更大的行为缺陷。由于女性在压力后更容易出现焦虑症,并且焦虑是由大麻素受体(CBRs)(CB1和CB2)介导的,因此需要比较在压力较大的男性和女性中CB1和CB2的表达。使用qPCR在连续3 d重复的尾巴震荡后3天,测定青春期雌雄大鼠杏仁核,海马,前额叶皮层(PFC)和下丘脑中CB1和CB2 mRNA的表达。使用蛋白质印迹技术确定PFC CB1和CB2蛋白水平。性别和压力均对脑CB1 mRNA表达水平有显着影响。总体而言,女性在所有大脑区域的CB1和CB2 mRNA水平均明显高于男性(p <0.01)。反复的压力降低了杏仁核,海马和PFC中CB1 mRNA的水平(每个p <0.01)。在海马(p <0.05),下丘脑(p <0.01)和PFC(p 2 蛋白水平均降低(p <0.05,各自)。幼稚的年轻女性中较高的基础CBR表达水平可以预防TBI损伤,而压力引起的CBR缺乏可能预示着反复受累女性中TBI的预后较差。进一步的动物研究可以帮助评估这种可能性。

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