首页> 外文期刊>Pharmacology, Biochemistry and Behavior >Chronic exposure to WIN55, 212-2 affects more potently spatial learning and memory in adolescents than in adult rats via a negative action on dorsal hippocampal neurogenesis
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Chronic exposure to WIN55, 212-2 affects more potently spatial learning and memory in adolescents than in adult rats via a negative action on dorsal hippocampal neurogenesis

机译:与成年大鼠相比,长期暴露于WIN55、212-2对青少年的空间学习和记忆的影响更大,这是通过对背侧海马神经发生的负面作用

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Several epidemiological studies show an increase in cannabis use among adolescents, especially in Morocco for being one of the major producers in the world. The neurobiological consequences of chronic cannabis use are still poorly understood. In addition, brain plasticity linked to ontogeny portrays adolescence as a period of vulnerability to the deleterious effects of drugs. The aim of this study was to investigate the behavioral neurogenic effects of chronic exposure to the cannabinoid agonist WIN55, 212-2 during adolescence, by evaluating the emotional and cognitive performances, and the consequences on neurogenesis along the dorso-ventral axis of the hippocampus in adult rats. WIN55, 212 was administered intraperitoneally (i.p.) once daily for 20 days to adolescent (27-30 PND) and adult Wistar rats (54-57 PND) at the dose of 1 mg/kg. Following a 20 day washout period, emotional and cognitive functions were assessed by the Morris water maze test and the two-way active avoidance test. Twelve hours after, brains were removed and hippocampal neurogenesis was assessed using the doublecortin (DCX) as a marker for cell proliferation. Our results showed that chronic WIN55, 212-2 treatment significantly increased thigmotaxis early in the training process whatever the age of treatment, induced spatial learning and memory deficits in adolescent but not adult rats in the Morris water maze test, while it had no significant effect in the active avoidance test during multitrial training in the shuttle box. In addition, the cognitive deficits assessed in adolescent rats were positively correlated to a decrease in the number of newly generated neurons in dorsal hippocampus. These data suggest that long term exposure to cannabinoids may affect more potently spatial learning and memory in adolescent compared to adult rats via a negative action on hippocampal plasticity.
机译:几项流行病学研究表明,青少年使用大麻的情况有所增加,特别是在摩洛哥,摩洛哥是世界上主要的生产国之一。长期使用大麻的神经生物学后果仍然知之甚少。此外,与个体发育有关的大脑可塑性将青春期描述为对药物有害作用的脆弱时期。这项研究的目的是通过评估其情绪和认知表现以及对沿海马背腹轴对神经发生的影响,研究青春期慢性接触大麻素激动剂WIN55、212-2的行为神经源性作用。成年大鼠。 WIN55,212腹膜内(i.p.)每天一次,剂量为1 mg / kg,对青春期(27-30 PND)和成年Wistar大鼠(54-57 PND)进行一次腹膜内给药(20天)。冲洗20天后,通过莫里斯水迷宫测试和双向主动回避测试评估情绪和认知功能。 12小时后,移开大脑,并使用双皮质激素(DCX)作为细胞增殖的标志物评估海马神经发生。我们的研究结果表明,无论治疗年龄多大,长期的WIN55、212-2治疗在训练过程的早期都显着增加了趋轴性,在莫里斯水迷宫测试中未引起成年大鼠的空间学习和记忆障碍,但对成年大鼠却没有影响。在穿梭箱中进行多次试训的主动回避测试中。此外,在青春期大鼠中评估的认知缺陷与背侧海马中新产生的神经元数量减少呈正相关。这些数据表明,与成年大鼠相比,长期暴露于大麻素可能会对海马可塑性产生负面影响,从而更有效地影响青少年的空间学习和记忆。

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