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成年鼠器官型海马脑片培养中细胞损伤的评估:研究神经保护的潜在模型系统。

Evaluation of cell damage in organotypic hippocampal slice culture from adult mouse: a potential model system to study neuroprotection.

机构信息

Key Laboratory of Neurogenetics and Channelopathies of Guangdong Province and Ministry of Education of China, Institute of Neuroscience and the Second Affiliated Hospital of Guangzhou Medical University, Guangzhou, China.

出版信息

Brain Res. 2011 Apr 18;1385:68-76. doi: 10.1016/j.brainres.2011.01.115.

Abstract

The use of organotypic hippocampal slice culture (OHSC) has become a powerful tool for studying cell damage in different neuropathological states, since it reproduces the basic morphological and functional properties of hippocampal neuronal network. However, the conventional OHSCs are established from postnatal animals rather than adult. Here we reevaluated the features of cell death in adult OHSC in detail and found potential utility for the study of neuroprotection. Organotypic culture of hippocampal slices from adult mice under conventional conditions led to a time-dependent and reproducible cell death. Around 6days in vitro (DIV), slices lost 50% of the cells, based on LDH release assessment. The cell death was greater than 90% after DIV 15. The cell loss was linearly correlated (r=0.944, P<0.01) with the time in culture. The electrophysiological responses to the stimulus in the cultured adult slices were accordingly reduced. The cell degeneration during adult OHSC might be utilized as a tool for studying neuroprotective effects in drug development. To illustrate this potential use, adult OHSCs were challenged with brain-derived neurotrophic factor (BDNF). We found that the continuous supplementation of 300ng/ml BDNF promoted cell survival of adult OHSC. Using immunohistochemistry and Western blot analyses of neuronal markers, we also demonstrated the pro-survival effects of BDNF on neurons in the adult OHSC system. It is suggested that OHSCs from adult mice might provide an alternative model system for neuronal degeneration, suitable for studying physiological factors and pharmacological compounds contributing to neuronal survival.

摘要

器官型海马脑片培养(OHSC)已成为研究不同神经病理学状态下细胞损伤的有力工具,因为它再现了海马神经元网络的基本形态和功能特性。然而,传统的 OHSCs 是由新生动物而不是成年动物建立的。在这里,我们详细重新评估了成年 OHSC 中细胞死亡的特征,并发现了其在神经保护研究中的潜在用途。在常规条件下,从成年小鼠中培养的海马脑片的器官型培养导致了时间依赖性和可重现的细胞死亡。基于 LDH 释放评估,在体外培养 6 天时,切片丧失了 50%的细胞。在 DIV15 后,细胞死亡超过 90%。细胞丢失与培养时间呈线性相关(r=0.944,P<0.01)。培养的成年脑片中对刺激的电生理反应相应降低。成年 OHSC 期间的细胞退化可能被用作研究药物开发中神经保护作用的工具。为了说明这种潜在的用途,我们用脑源性神经营养因子(BDNF)挑战成年 OHSCs。我们发现,持续补充 300ng/ml 的 BDNF 可促进成年 OHSC 的细胞存活。通过对神经元标志物的免疫组织化学和 Western blot 分析,我们还证明了 BDNF 对成年 OHSC 系统中神经元的生存促进作用。因此,来自成年小鼠的 OHSCs 可能为神经元退化提供了另一种替代模型系统,适合研究促进神经元存活的生理因素和药物化合物。

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