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Prenatal stress-induced impairments of cognitive flexibility and bidirectional synaptic plasticity are possibly associated with autophagy in adolescent male-offspring

机译:产前应激诱导的认知灵活性和双向突触塑性的损伤可能与青少年男性后代的自噬有关

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Prenatal stress (PS) brings numerous outcomes on offspring, including anxiety, depression-like behavior and other cognitive disorder. In this study, a rat model of PS was established by using restraint stress for 45 min three times per day from the 15th to 21st day of pregnancy. Behavioral tests, including open field test (OPT), elevated plus-maze (EPM) and Morris water-maze (MWM), were performed in adolescent male-offspring. The bidirectional synaptic plasticity, including long-term potential (LTP) and depotentiation (DEP), from the hippocampal Schaffer collaterals to CA1 region was subsequently measured. Furthermore, Western blot assay, immunofluorescence staining and hematoxylin-eosin (HE) staining were employed. The MWM test showed that the cognitive flexibility was remarkably damaged in PS offspring. Meanwhile, PS considerably aggravated the anxiety and depression-like behavior in OPT and EPM. Both LTP and DEP were significantly inhibited by PS. Furthermore, PS considerably altered the expression of synaptic-related proteins NR2A, NR2B and PSD-95 in adolescent male-offspring. Interestingly, PS significantly elevated the autophagy level in the hippocampus of male-offspring. In order to investigate the role of autophagy on the negative impacts of PS in adolescent male-offspring, both in vitro and in vivo studies were performed. It was found that autophagy inhibitors significantly eliminated the alterations in gene expression induced by corticosterone. The results suggest that regulating autophagy may become a new targeted therapy to relieve the damage induced by PS in adolescent male-off-spring.
机译:产前压力(PS)为后代带来了许多结果,包括焦虑,抑郁的行为和其他认知障碍。在这项研究中,通过从第15至第21天的妊娠,通过使用约束应力为每天45分钟的抑制应力来确定PS的大鼠模型。在青少年雄性后代进行行为测试,包括开场测试(选择),升高的加迷宫(EPM)和Morris水迷宫(MWM)。随后测量双向突触可塑性,包括长期电位(LTP)和沉积(DEP),从海马Schaffer侧面到Ca1区。此外,使用蛋白质印迹测定,免疫荧光染色和苏木精 - 曙红(HE)染色。 MWM试验表明,在PS后代,认知灵活性显着受损。与此同时,PS大大加剧了OPT和EPM中的焦虑和抑郁的行为。 LTP和DEP都被PS显着抑制。此外,PS大大改变了青少年雄性后代突触相关蛋白NR2A,NR2B和PSD-95的表达。有趣的是,PS显着升高了男性后代海马的自噬水平。为了探讨自噬作用对青少年男性后代PS对PS的负面影响,在体外和体内研究中进行。发现自噬抑制剂显着消除了皮质酮诱导的基因表达的改变。结果表明,调节自噬可能成为一种新的靶向治疗,以缓解PS在青少年阳性春季PS中PS诱导的损伤。

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