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发育中大鼠海马内注射红藻氨酸后的神经元丢失、苔藓纤维发芽和发作间期棘波

Neuron loss, mossy fiber sprouting, and interictal spikes after intrahippocampal kainate in developing rats.

作者信息

Leite J P, Babb T L, Pretorius J K, Kuhlman P A, Yeoman K M, Mathern G W

机构信息

Brain Research Institute, University of California, Los Angeles, USA.

出版信息

Epilepsy Res. 1996 Dec;26(1):219-31. doi: 10.1016/s0920-1211(96)00055-1.

Abstract

This study determined neuron losses, mossy fiber sprouting, and interictal spike frequencies in adult rats following intrahippocampal kainic acid (KA) injections during postnatal (PN) development. KA (0.4 micrograms/0.2 microliters; n = 64) was injected into one hippocampus and saline into the contralateral side between PN 7 to 30 days. Animals were sacrificed 28 to 256 days later, along with age-matched naive animals (controls; n = 20). Hippocampi were studied for: (1) Fascia dentata granule cell, hilar, and CA3c neuron counts; (2) neo-Timm's stained supragranular mossy fiber sprouting; and (3) hippocampal and intracerebral interictal spike densities (n = 13). Mossy fiber sprouting was quantified as the gray value differences between the inner and outer molecular layer. Statistically significant results (p < 0.05) showed the following: (1) Compared to controls, CA3c and hilar neuron counts were reduced in KA-hippocampi with injections at PN 7-10 and PN 12-14 respectively and counts decreased with older PN injections. Granule cell densities on the KA-side and saline injected hippocampi were not reduced compared to controls. (2) In adult rats, supragranular mossy fiber sprouting was observed in 2 of 7 PN 7 injected animals. Compared to controls, increased gray value differences, indicating mossy fiber sprouting, were found on the KA-side beginning with injuries at PN 12-14 and increasing with older PN injections. On the saline-side only PN 30 animals showed minimal sprouting. (3) Mossy fiber sprouting progressively increased on the KA-side with longer survivals in rats injured after PN 15. Sprouting correlated positively with later PN injections and longer post-injection survival intervals, and not with reduced hilar or CA3c neuron counts. (4) On the KA-side, mossy fiber gray value differences correlated positively with in vivo intrahippocampal interictal spike densities. These results indicate that during postnatal rat development intrahippocampal kainate excitotoxicity can occur as early as PN 7 and increases with older ages at injection. This rat model reproduces many of the pathologic, behavioral, and electrophysiologic features of human mesial temporal lobe epilepsy, and supports the hypothesis that hippocampal sclerosis can be the consequence of focal injury during early postnatal development that progressively evolves into a pathologic and epileptic focus.

摘要

本研究确定了出生后(PN)发育期间海马内注射 kainic 酸(KA)的成年大鼠的神经元损失、苔藓纤维发芽和发作间期棘波频率。在 PN 7 至 30 天之间,将 KA(0.4 微克/0.2 微升;n = 64)注入一侧海马,对侧注入生理盐水。28 至 256 天后处死动物,同时处死年龄匹配的未处理动物(对照组;n = 20)。对海马进行以下研究:(1)齿状回颗粒细胞、海马门和 CA3c 神经元计数;(2)新 Timm 染色的颗粒上层苔藓纤维发芽;(3)海马和脑内发作间期棘波密度(n = 13)。苔藓纤维发芽通过分子层内外的灰度值差异进行量化。具有统计学意义的结果(p < 0.05)如下:(1)与对照组相比,分别在 PN 7 - 10 和 PN 12 - 14 注射 KA 的海马中,CA3c 和海马门神经元计数减少,且随着 PN 注射年龄增大,计数降低。与对照组相比,KA 侧和注射生理盐水侧的海马颗粒细胞密度未降低。(2)在成年大鼠中,7 只在 PN 7 注射的动物中有 2 只观察到颗粒上层苔藓纤维发芽。与对照组相比,从 PN 12 - 14 损伤开始,KA 侧的灰度值差异增加,表明苔藓纤维发芽,且随着 PN 注射年龄增大而增加。在生理盐水侧,只有 PN 30 的动物表现出最小程度的发芽。(3)在 PN 15 后受伤的大鼠中,随着存活时间延长,KA 侧的苔藓纤维发芽逐渐增加。发芽与较晚的 PN 注射和较长的注射后存活间隔呈正相关,与海马门或 CA3c 神经元计数减少无关。(4)在 KA 侧,苔藓纤维灰度值差异与体内海马发作间期棘波密度呈正相关。这些结果表明,在出生后大鼠发育期间,海马内 kainate 兴奋性毒性最早可在 PN 7 时发生,并随着注射年龄增大而增加。该大鼠模型重现了人类内侧颞叶癫痫的许多病理、行为和电生理特征,并支持以下假设:海马硬化可能是出生后早期发育期间局灶性损伤的结果,该损伤逐渐演变为病理和癫痫病灶。

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