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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Characterisation of cell damage and death in embryonic mesencephalic tissue: a study on ultrastructure, vital stains and protease activity.
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Characterisation of cell damage and death in embryonic mesencephalic tissue: a study on ultrastructure, vital stains and protease activity.

机译:胚胎中脑组织中细胞损伤和死亡的特征:超微结构,重要染色和蛋白酶活性的研究。

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Dissociated embryonic ventral mesencephalic tissue is a source of dopaminergic neurones in both cell culture and neural transplantation studies. Around 90% of grafted dopaminergic neurones die within 1 week after transplantation. Little is known about when the cell death is triggered and what forms of cell death predominate. Using electron microscopy, we characterised ultrastructural changes in dissected embryonic day 14 rat mesencephalic tissue before and after tissue dissociation. In addition, cell viability was evaluated using Trypan Blue and Hoechst/Ethidium Homodimer. Several cells exhibited leaky outer membranes (permitting entry of vital stains) and ultrastructural degeneration already immediately after the mesencephalon was dissected, and before it was mechanically disrupted. After 2 h at room temperature, 90% of the remaining cells had intact outer membranes. However, when estimating cells lost acutely in the tissue dissociation, in addition to cells exhibiting condensed chromatin and organellar changes, we suggest that only around 14% of the cells initially dissected in the mesencephalic tissue pieces remained healthy after 2 h. There was a peak in calpain activity (specific cleavage of fodrin) immediately following tissue dissociation, and it subsided during the next few hours. Caspase-3 activity was initially low, but increased almost 20-fold 4 h after tissue disruption. Interestingly, extensive degradation of caspase-3 occurred already directly after dissection and was at least partly calpain-dependent. Our data suggest that, in addition to cells undergoing primary necrosis, some cells undergo apoptotic or related changes soon after tissue harvesting, and eventually undergo a secondary necrosis. In summary, embryonic mesencephalic cells exhibit multiple degenerative changes very early on in the neural transplant/tissue culture preparation protocol.
机译:在细胞培养和神经移植研究中,离体的胚胎腹侧中脑组织都是多巴胺能神经元的来源。移植后1周内约有90%的移植多巴胺能神经元死亡。对于何时触发细胞死亡以及什么形式的细胞死亡占主导地位,人们知之甚少。使用电子显微镜,我们表征了组织解离前后的解剖胚胎第14天大鼠中脑组织的超微结构变化。此外,使用锥虫蓝和Hoechst / Ethidium Homodimer评估细胞活力。在中脑被解剖后和机械破坏之前,已经有几个细胞表现出渗漏的外膜(允许进入活菌斑)和超微结构变性。在室温下2小时后,其余90%的细胞具有完整的外膜。但是,当估计细胞在组织解离中急剧丢失时,除了显示出染色质和细胞器质凝集浓缩的细胞外,我们建议仅在中脑组织碎片中最初解剖的细胞中约有14%在2 h后仍保持健康。组织解离后,钙蛋白酶活性(铁蛋白的特异性裂解)立即达到峰值,并在接下来的几个小时内平息。 Caspase-3活性最初较低,但在组织破裂后4小时增加了近20倍。有趣的是,解剖后直接发生了caspase-3的大量降解,并且至少部分依赖钙蛋白酶。我们的数据表明,除细胞遭受原发性坏死外,某些细胞在组织收获后不久会发生凋亡或相关变化,并最终发生继发性坏死。总之,胚胎中脑细胞在神经移植/组织培养物制备方案中很早就表现出多种变性变化。

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