Remigio Gregory J, Loewen Jaycie L, Heuston Sage, Helgeson Colin, White H Steve, Wilcox Karen S, West Peter J
Interdepartmental Neuroscience Program, University of Utah, Salt Lake City, UT 84108-1210, USA; Department of Pharmacology and Toxicology, University of Utah, Salt Lake City, UT 84108-1210, USA.
The Waterford School, Sandy, UT 84093-2902, USA.
Neurobiol Dis. 2017 Sep;105:221-234. doi: 10.1016/j.nbd.2017.06.006. Epub 2017 Jun 15.
Memory deficits have a significant impact on the quality of life of patients with epilepsy and currently no effective treatments exist to mitigate this comorbidity. While these cognitive comorbidities can be associated with varying degrees of hippocampal cell death and hippocampal sclerosis, more subtle changes in hippocampal physiology independent of cell loss may underlie memory dysfunction in many epilepsy patients. Accordingly, animal models of epilepsy or epileptic processes exhibiting memory deficits in the absence of cell loss could facilitate novel therapy discovery. Mouse corneal kindling is a cost-effective and non-invasive model of focal to bilateral tonic-clonic seizures that may exhibit memory deficits in the absence of cell loss. Therefore, we tested the hypothesis that corneal kindled C57BL/6 mice exhibit spatial pattern processing and memory deficits in a task reliant on DG function and that these impairments would be concurrent with physiological remodeling of the DG as opposed to overt neuron loss. Following corneal kindling, C57BL/6 mice exhibited deficits in a DG-associated spatial memory test - the metric task. Compatible with this finding, we also discovered saturated, and subsequently impaired, LTP of excitatory synaptic transmission at the perforant path to DGC synapse. This saturation of LTP was consistent with evidence suggesting that perforant path to DGC synapses in kindled mice had previously experienced LTP-like changes to their synaptic weights: increased postsynaptic depolarizations in response to equivalent presynaptic input and significantly larger amplitude AMPA receptor mediated spontaneous EPSCs. Additionally, there was evidence for kindling-induced changes in the intrinsic excitability of DGCs: reduced threshold to population spikes under extracellular recording conditions and significantly increased membrane resistances observed in DGCs. Importantly, quantitative immunohistochemical analysis revealed hippocampal astrogliosis in the absence of overt neuron loss. These changes in spatial pattern processing and memory deficits in corneal kindled mice represent a novel model of seizure-induced cognitive dysfunction associated with pathophysiological remodeling of excitatory synaptic transmission and granule cell excitability in the absence of overt cell loss.
记忆缺陷对癫痫患者的生活质量有重大影响,目前尚无有效的治疗方法来缓解这种合并症。虽然这些认知合并症可能与不同程度的海马体细胞死亡和海马硬化有关,但在许多癫痫患者中,独立于细胞丢失的海马生理更细微变化可能是记忆功能障碍的基础。因此,在无细胞丢失情况下表现出记忆缺陷的癫痫动物模型或癫痫过程模型可能有助于发现新的治疗方法。小鼠角膜点燃是一种具有成本效益的非侵入性局灶性至双侧强直阵挛性癫痫模型,在无细胞丢失的情况下可能表现出记忆缺陷。因此,我们检验了以下假设:角膜点燃的C57BL/6小鼠在依赖齿状回(DG)功能的任务中表现出空间模式处理和记忆缺陷,并且这些损伤将与DG的生理重塑同时发生,而不是明显的神经元丢失。角膜点燃后,C57BL/6小鼠在与DG相关的空间记忆测试——度量任务中表现出缺陷。与此发现一致,我们还发现了在穿通通路至齿状回颗粒细胞(DGC)突触处兴奋性突触传递的长时程增强(LTP)饱和,随后受损。这种LTP的饱和与证据一致,表明点燃小鼠中穿通通路至DGC突触先前已经历其突触权重的类似LTP的变化:对等效突触前输入的反应中突触后去极化增加,以及AMPA受体介导的自发性兴奋性突触后电流(EPSCs)幅度显著增大。此外,有证据表明点燃诱导了DGCs内在兴奋性的变化:在细胞外记录条件下群体峰电位的阈值降低,并且在DGCs中观察到膜电阻显著增加。重要的是,定量免疫组织化学分析显示在无明显神经元丢失的情况下海马星形胶质细胞增生。角膜点燃小鼠的这些空间模式处理和记忆缺陷的变化代表了一种新的癫痫诱导的认知功能障碍模型,其与兴奋性突触传递和颗粒细胞兴奋性的病理生理重塑相关,而无明显细胞丢失。
