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TNF-alpha secretion and apoptosis of lymphocytes mediated by gene transfer.

机译:基因转移介导的淋巴细胞的TNF-α分泌和凋亡。

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Efficient gene transfer of lymphocytes is extremely difficult. Apoptosis may play a role in this gene transfer resistance of lymphocytes. Here we show that transfection of lymphocytes via non-viral vectors leads to induction of apoptosis in a significant proportion of cells. Since apoptosis may be mediated via tumor necrosis factor d (TNF-alpha) and the TNF-alpha receptor pathway, we studied the amount of TNF-alpha secreted by lymphocytes transfected without gene insert. TNF-alpha secretion was dependent on the gene transfer method used. High amounts were detected using receptor-mediated gene transfer and lipofection. In contrast, only low amounts of TNF-alpha were detected after electroporation and retroviral gene transfer. In receptor-mediated gene transfer, TNF-alpha secretion was due to the use of anti-CD3 antibody. Transfection of lymphocytes led to selective decrease in CD120b/TNF-alpha receptor II (TNFR-2)-positive cells. Induction of apoptosis and necrosis mediated by TNF-alpha via TNFR-2 (p80) was partially blocked using a neutralizing anti-TNF-alpha antibody. Blockage of apoptosis and necrosis could be further increased by adding anti-Fas-ligand (FasL) antibody, suggesting that induction of apoptosis via FasL and Fas receptor (Apo-1/CD95) may also play a role. This blockage led to a significant increase in the proliferation rate of lymphocytes transfected with cytokine genes. In conclusion, various gene transfer techniques led to TNF-alpha secretion, apoptosis and necrosis of lymphocytes. Apoptosis and necrosis could be partially blocked using a neutralizing anti-TNF-alpha antibody.
机译:淋巴细胞的有效基因转移非常困难。凋亡可能在淋巴细胞的这种基因转移抗性中起作用。在这里,我们显示了通过非病毒载体转染淋巴细胞导致大量细胞凋亡的诱导。由于凋亡可能是通过肿瘤坏死因子d(TNF-α)和TNF-α受体途径介导的,因此我们研究了未经基因插入的转染淋巴细胞分泌的TNF-α的数量。 TNF-α分泌取决于所使用的基因转移方法。使用受体介导的基因转移和脂质转染检测到大量。相反,电穿孔和逆转录病毒基因转移后仅检测到少量的TNF-α。在受体介导的基因转移中,TNF-α分泌是由于使用了抗CD3抗体。淋巴细胞的转染导致CD120b /TNF-α受体II(TNFR-2)阳性细胞的选择性减少。使用中和性抗TNF-α抗体可部分阻断TNF-α通过TNFR-2(p80)介导的凋亡和坏死的诱导。加入抗Fas-配体(FasL)抗体可进一步增加细胞凋亡和坏死的阻滞,提示通过FasL和Fas受体(Apo-1 / CD95)诱导细胞凋亡也可能起一定作用。这种阻断导致被细胞因子基因转染的淋巴细胞的增殖速率显着增加。总之,各种基因转移技术导致TNF-α分泌,淋巴细胞凋亡和坏死。使用中和性抗TNF-α抗体可以部分阻断细胞凋亡和坏死。

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