首页> 美国卫生研究院文献>Frontiers in Behavioral Neuroscience >Consequences of Adolescent Exposure to the Cannabinoid Receptor Agonist WIN55212-2 on Working Memory in Female Rats
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Consequences of Adolescent Exposure to the Cannabinoid Receptor Agonist WIN55212-2 on Working Memory in Female Rats

机译:青少年暴露于大麻受体激动剂WIN55212-2对雌性大鼠工作记忆的后果

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摘要

Marijuana is a prevalent illicit substance used by adolescents, and several studies have indicated that adolescent use can lead to long-term cognitive deficits including problems with attention and memory. However, preclinical animal studies that observe cognitive deficits after cannabinoid exposure during adolescence utilize experimenter administration of doses of cannabinoids that may exceed what an organism would choose to take, suggesting that contingency and dose are critical factors that need to be addressed in translational models of consequences of cannabinoid exposure. Indeed, we recently developed an adolescent cannabinoid self-administration paradigm in male rats, and found that prior adolescent self-administration of the cannabinoid receptor agonist WIN55,212-2 (WIN) resulted in improved working memory performance in adulthood. In addition, the doses self-administered were not as high as those that are found to produce memory deficits. However, given known sex differences in both drug self-administration and learning and memory processes, it is possible that cannabinoid self-administration could have different cognitive consequences in females. Therefore, we aimed to explore the effects of self-administered vs. experimenter-administered WIN in adolescent female rats on adult cognitive function. Female rats were trained to self-administer WIN daily throughout adolescence (postnatal day 34–59). A control group self-administered vehicle solution. The acute effects of adolescent WIN self-administration on memory were determined using a short-term spatial memory test 24 h after final SA session; and the long-term effects on cognitive performance were assessed during protracted abstinence in adulthood using a delayed-match-to-sample working memory task. In a separate experiment, females were given daily intraperitoneal (IP) injections of a low or high dose of WIN, corresponding to self-administered and typical experimenter-administered doses, respectively, or its vehicle during adolescence and working memory was assessed under drug-free conditions in adulthood. While self-administration of WIN in adolescence had no significant effects on short-term spatial memory or adult working memory, experimenter administration of WIN resulted in improved adult working memory performance that was more pronounced in the low dose group. Thus, low-dose adolescent WIN exposure, whether self-administered or experimenter-administered, results in either improvements or no change in adult working memory performance in female rats, similar to previous results found in males.
机译:大麻是青少年普遍使用的非法物质,一些研究表明,青少年使用大麻会导致长期的认知缺陷,包括注意力和记忆力问题。但是,临床前动物研究观察了青春期接触大麻素后的认知缺陷,该实验利用实验人员给予的大麻素剂量可能超过生物体会选择的剂量,这表明偶然性和剂量是后果转化模型中需要解决的关键因素大麻暴露。的确,我们最近在雄性大鼠中开发了一种青春期大麻素自我给药范例,并发现先前的青春期大麻素受体激动剂WIN55,212-2(WIN)自我给药可改善成年期的工作记忆性能。另外,自我给药的剂量不如发现会产生记忆缺陷的剂量高。但是,鉴于在药物自我管理以及学习和记忆过程中已知的性别差异,大麻素自我管理可能会对女性产生不同的认知后果。因此,我们旨在探讨青春期雌性大鼠中自我给药与实验人员给药的WIN对成年认知功能的影响。训练雌性大鼠在整个青春期(产后第34-59天)每天进行WIN自我管理。对照组自我管理的车辆解决方案。在最后一次SA疗程后24小时,通过短期空间记忆测试确定了青少年WIN自我管理对记忆的急性影响;并通过延迟匹配样本工作记忆任务评估了成年后长期禁欲期间对认知能力的长期影响。在另一项实验中,每天分别给雌性大鼠腹膜内(IP)注射低剂量或高剂量的WIN,分别对应于自身给药和典型实验者给药的剂量,或者在青春期和工作记忆下使用药物进行评估成年时期的自由条件。青春期服用WIN自我管理对短期空间记忆或成人工作记忆没有显着影响,而WIN的实验者管理导致成年人工作记忆性能的改善,在低剂量组中更为明显。因此,低剂量的青少年WIN暴露,无论是自我给药还是实验人员给药,都会导致雌性大鼠的成年工作记忆性能得到改善或没有变化,这与雄性大鼠先前的结果相似。

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