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Effect of lentivirus-mediated survivin transfection on the morphology and apoptosis of nucleus pulposus cells derived from degenerative human disc in vitro

机译:慢病毒介导的survivin转染对体外变性人椎间盘髓核细胞形态和凋亡的影响

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摘要

Lower back pain is a common concern, and 40% of all cases involve the degeneration of the intervertebral disc (IVD). However, the excessive apoptosis of disc cells plays an important role in IVD degeneration, particularly in the nucleus pulposus (NP). Thus, anti-apoptotic gene therapy to attenuate or reverse the degenerative process within the NP is being developed. Survivin is a unique inhibitor of apoptosis (IAP) and has been extensively investigated in cancer cells. However, little is known of the effects of survivin transfection on NP cells derived from degenerative human disc. In this study, we aimed to investigate the effects of lentivirus (LV)-mediated survivin transfection on the morphology and apoptosis of NP cells derived from degenerative human disc in vitro. NP cells were transfected with LV-mediated survivin. Subsequently, cell morphology was observed and the survivin mRNA expression levels were measured by RT-qPCR. Apoptosis was analyzed by flow cytometry and by measuring caspase-3 activity. The results revealed that the morphology of the NP cells derived from degenerative human disc transfected with LV-mediated survivin was significantly altered as evidenced by cytomorphosis, the reduction of the cytoplasm and cell shrinkage. Following transfection, survivin gene expression significantly increased in the transfected cells and subsequent generation cells; however, no significant differences in the cell apoptotic rate and caspase-3 activity were observed. We found that transfection of the survivin gene into NP cells led to the stable expression of survivin and induced marked changes in cell morphology. Furthermore, no significant anti-apoptotic effects were observed following LV-mediated survivin transfection. Overall, our findings demonstrate that LV carrying surviving may be used to successfully enforce the expression of survivin in NP cells. However, cell morphology was evidently altered, whereas the apoptotic rate did not decrease. Comprehensive studies on the feasibility of using survivin in gene therapy in an aim to attenuate disc degeneration are warranted. Further research on the mechanisms responsible for the changes in cell morphology and cell function are also required.
机译:下背部疼痛是一个常见的问题,所有病例中有40%涉及椎间盘(IVD)变性。但是,椎间盘细胞过度凋亡在IVD变性中起着重要作用,尤其是在髓核(NP)中。因此,正在开发抗凋亡基因疗法以减弱或逆转NP内的退化过程。 Survivin是独特的凋亡抑制剂(IAP),已经在癌细胞中进行了广泛研究。然而,关于存活蛋白转染对衍生自变性人椎间盘的NP细胞的影响知之甚少。在这项研究中,我们旨在调查慢病毒(LV)介导的survivin转染对体外变性人椎间盘NP细胞形态和凋亡的影响。用LV介导的survivin转染NP细胞。随后,观察细胞形态并通过RT-qPCR测量survivin mRNA表达水平。通过流式细胞术和通过测量caspase-3活性来分析细胞凋亡。结果表明,如细胞形态,细胞质减少和细胞皱缩所证实,用LV介导的survivin转染的变性人椎间盘衍生的NP细胞的形态发生了显着改变。转染后,survivin基因表达在转染细胞和后代细胞中显着增加。然而,在细胞凋亡率和caspase-3活性方面没有观察到显着差异。我们发现survivin基因转染到NP细胞中导致survivin的稳定表达并诱导细胞形态发生明显变化。此外,在LV介导的survivin转染后未观察到显着的抗凋亡作用。总体而言,我们的研究结果表明携带LV的幸存者可用于成功地增强survivin在NP细胞中的表达。然而,细胞形态明显改变,而细胞凋亡率并未降低。有必要对在基因治疗中使用survivin来减轻椎间盘退变的可行性进行全面研究。还需要进一步研究负责细胞形态和细胞功能变化的机制。

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