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Role of hippocampal nitrergic neurotransmission in behavioral and cardiovascular dysfunctions evoked by chronic social stress

机译:海马硝态能神经递质在慢性社会压力引起行为和心血管功能障碍中的作用

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Increased nitric oxide (NO) levels have been identified in the hippocampus of animals subjected to social isolation. However, a role of this change in behavioral and physiological changes evoked by isolation has never been evaluated. Thus, this study investigated the involvement of nitrergic neurotransmission acting via the neuronal isoform of nitric oxide synthase (nNOS) within the dorsal hippocampus in behavioral and cardiovascular changes in isolated reared rats. For this, male rats were isolated from weaning at 21 days postnatal for 40 days. We identified that social isolation increased hippocampal NO formation and nNOS expression. Besides, anxiogenic- and depressive-like effect identified in isolated animals were not affected by intra-hippocampal microinjection of either the NO scavenger carboxy-PTIO or the selective nNOS inhibitor N-omega-Propyl-L-arginine (NPLA). Isolation also increased basal arterial pressure, impaired the baroreflex function and decreased the tachycardia to restraint stress. The effects in restraint-evoked tachycardia were inhibited by hippocampal treatment with either carboxy-PTIO or NPLA. Intra-hippocampal administration of either carboxy-PTIO or NPLA also enhanced the pressor response to restraint in isolated, but not in control animals. Taken together, these findings indicate that increased NO release within the dorsal hippocampus is involved in impairment of cardiovascular responses to a novel stressor, but not in behavioral effects and baroreflex changes, evoked by social isolation. Furthermore, exposure to this stressor evokes the emergence of an inhibitory role of hippocampal nNOS activation in cardiovascular changes to a novel stressor, which might constitute a prominent adaptive response.
机译:在受到社会隔离的动物的海马海马中鉴定了一氧化氮(NO)水平。然而,从未评估过诱导这种发生这种变化的作用和生理变化的作用。因此,本研究调查了在分离的饲养大鼠的行为和心血管变化中通过一氧化氮合酶(NNOS)内氧化氮合酶(NNOS)内的神经元同种扫描作用的纳撒式神经递血。为此,在第21天的后,将雄性大鼠从断奶中分离出来40天。我们认为社会隔离增加了海马没有形成和NNOS表达。此外,在分离的动物中鉴定的焦虑和抑郁的效果不受NO清除剂羧基-PTIO或选择性NNOS抑制剂N-Omega-Propyl-L-精氨酸(NPLA)的内移式显微注射的影响。分离也增加了基础动脉压力,损伤了骨折函数并降低了心动过速降低了压力。通过用羧基-PTIO或NPLA进行海马治疗抑制诱发的心动过速的影响。羧基-PTIO或NPLA的海豚药物施用还增强了对隔离的克制的压力机响应,但不在对照动物中。在一起,这些发现表明,越来越多的海马内没有释放涉及对新型压力源的心血管反应的损害,但不受社会隔离的行为效应和苦恼的变化。此外,暴露于该压力源引起海马NNOS活化在心血管变化对新型压力源的抑制作用的出现,这可能构成突出的适应性反应。

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