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首页> 外文期刊>Journal of the Neurological Sciences: Official Bulletin of the World Federation of Neurology >Ischemic preconditioning inhibits expression of Na~+/H~+ exchanger 1 (NHE1) in the gerbil hippocampal CA1 region after transient forebrain ischemia
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Ischemic preconditioning inhibits expression of Na~+/H~+ exchanger 1 (NHE1) in the gerbil hippocampal CA1 region after transient forebrain ischemia

机译:缺血预处理抑制短暂性前脑缺血后沙鼠海马CA1区Na〜+ / H〜+交换子1(NHE1)的表达

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摘要

The participation of Na~+/H~+ exchanger (NHE) in neuronal damage/death in the hippocampal CA1 region (CA1) induced by transient forebrain ischemia has not been well established, although acidosis may be involved in neuronal damage/death. In the present study, we examined the effect of ischemic preconditioning (IPC) on NHE1 immunoreactivity following a 5 min of transient forebrain ischemia in gerbils. The animals used in the study were randomly assigned to four groups (sham-operated-group, ischemia-operated-group, IPC plus ( + ) sham-operated-group and IPC + ischemia-operated-group). IPC was induced by subjecting animals to 2 min of ischemia followed by 1 day of recovery. A significant neuronal loss was found in the stratum pyramidale (SP) of the CA1, not the CA2/3, of the ischemia-operated-group at 5 days post-ischemia. However, in the IPC + ischemia-operated-group, neurons in the SP of the CA1 were well protected. NHE1 immunoreactivity was not detected in any regions of the CA1-3 of the sham- and IPC + sham-operated-groups. However, the immunoreactivity was apparently expressed in the SP of the CA1-3 after ischemia, and the NHE1 immunoreactivity was very weak 5 days after ischemia; however, at this point in time, strong NHE1 immunoreactivity was found in astrocytes in the CA1. In the CA2/3, NHE1 immunoreactivity was slightly changed, although NHE1 immunoreactivity was expressed in the SP. In the IPC + ischemia-operated-groups, NHE1 immunoreactivity was also expressed in the SP of the CA1-3; however, the immunoreactivity was more slightly changed than that in the ischemia-operated-groups. In brief, our findings show that IPC dramatically protected CA1 pyramidal neurons and strongly inhibited NHE1 expression in the SP of the CA1 after ischemia-reperfusion. These findings suggest that the inhibition of NHE1 expression may be necessary for neuronal survival from transient ischemic damage.
机译:尽管酸中毒可能参与了神经元的损伤/死亡,但是Na + + / H +交换子(NHE)参与暂时性前脑缺血引起的海马CA1区(CA1)的神经元损伤/死亡的参与尚不充分。在本研究中,我们检查了沙土鼠短暂前脑缺血5分钟后缺血预处理(IPC)对NHE1免疫反应性的影响。研究中使用的动物被随机分为四组(假手术组,缺血手术组,IPC加(+)假手术组和IPC +缺血手术组)。通过对动物进行2分钟的缺血再恢复1天来诱导IPC。在缺血后5天,在缺血手术组的CA1而不是CA2 / 3的锥体层(SP)中发现了明显的神经元丢失。但是,在IPC +缺血操作组中,CA1 SP中的神经元受到了很好的保护。在假手术组和IPC +假手术组的CA1-3的任何区域均未检测到NHE1免疫反应性。然而,缺血后CA1-3的SP中明显表达了免疫反应性,缺血5天后NHE1免疫反应性非常弱。然而,在这一点上,在CA1的星形胶质细胞中发现了强烈的NHE1免疫反应性。在CA2 / 3中,尽管NHE1免疫反应性在SP中表达,但NHE1免疫反应性略有变化。在IPC +缺血操作组中,NHE1免疫反应性也在CA1-3的SP中表达。但是,免疫反应性比缺血手术组稍有改变。简而言之,我们的研究结果表明,缺血再灌注后IPC可以极大地保护CA1锥体神经元并强烈抑制CA1 SP中NHE1的表达。这些发现表明,NHE1表达的抑制对于短暂性脑缺血损伤的神经元存活可能是必需的。

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