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Characterization of embryonic cortical neuron death in prolonged cell suspension

机译:长时间悬浮细胞中胚胎皮质神经元死亡的特征

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摘要

Cell transplantation may be an effective therapeutic strategy for many neurodegenerative diseases. However, difficulty in obtaining a sufficient amount of donor cells and low graft survival are two major limiting factors. Dissociation of cells from tissues or culture is an inevitable step for cell transplantation, and cell viability in suspension may influence the outcome of the cell therapy. To this end, we asked whether the suspension time of freshly dissociated neurons in vitro affects their viability. Following 4-24. h cell suspension, primary cortical neurons underwent cell death. Interestingly, the neurons exhibited only marginal caspase-3 immunoreactivity with very few sub-G1 apoptotic cell proportions in flow cytometry. In addition, the suppression of caspase-3 or Bax action failed to prevent cell death of primary cortical neurons, indicating minimal apoptotic cell death. On the other hand, there was a marked increase in the TdT-mediated dUTP nick end labeling-positive and propidium iodide-labeled necrotic cells (~50%) with enhanced poly [ADP-ribose] polymerase-1 activity. Therefore, prevention against necrosis rather than apoptosis may be required for optimal benefits in cell transplantation.
机译:细胞移植可能是许多神经退行性疾病的有效治疗策略。然而,难以获得足够数量的供体细胞和低的移植物存活率是两个主要限制因素。细胞从组织或培养物中解离是细胞移植的必然步骤,并且细胞在悬浮液中的生存能力可能会影响细胞治疗的结果。为此,我们询问新鲜离解的神经元在体外的悬浮时间是否会影响其生存能力。以下4-24。细胞悬浮后,原代皮层神经元细胞死亡。有趣的是,在流式细胞仪中,神经元仅表现出少量的caspase-3免疫反应性,而亚G1凋亡细胞的比例却很少。此外,caspase-3或Bax活性的抑制未能阻止原代皮层神经元的细胞死亡,表明凋亡细胞的死亡极少。另一方面,具有增强的聚[ADP-核糖]聚合酶-1活性的TdT介导的dUTP缺口末端标记阳性和碘化丙啶标记的坏死细胞显着增加(〜50%)。因此,可能需要预防坏死而不是凋亡,以获得细胞移植的最佳益处。

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