首页> 外文期刊>Immunobiology: Zeitschrift fur Immunitatsforschung >Antitumor efficacy induced by human ovarian cancer cells secreting IL-21 alone or combination with GM-CSF cytokines in nude mice model.
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Antitumor efficacy induced by human ovarian cancer cells secreting IL-21 alone or combination with GM-CSF cytokines in nude mice model.

机译:在裸鼠模型中,人卵巢癌细胞单独分泌IL-21或与GM-CSF细胞因子组合诱导的抗肿瘤功效。

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The ovarian cancer cells (SKOV3) secreting IL-21 alone or combination with GM-CSF cytokines was developed and its antitumor effect was evaluated in the nude mice. The gene of IL-21 was amplified from plasmid pRSC-IL-21 by PCR, cloned into the plasmid pRSC-GM-CSF, and the plasmid pRSC-GM-CSF-IL21 was constructed. The plasmids of pRSC-GM-CSF, pRSC-IL21, pRSC-GM-CSF-IL21 and pRSC were respectively transfected into the SKOV3 cells and antitumor efficacy induced by the SKOV3 cells secreting IL-21 or combination with GM-CSF was evaluated by surveying the tumor growth and the nude mice's survival. The results indicated that the secreted IL-21 and GM-CSF were functional because the culture supernatant of SKOV3 cells transfected with the plasmid pRSC-GM-CSF-IL21 enhanced NK cytotoxicity in vitro. The expressions of MIC A/B, NKG2D and ICAM-1 molecules on the SKOV3 cells were up-regulated. The level of IFN-gamma and TNF-alpha, the NK cytotoxicity and the antitumor efficacy were significantly increased in the null mice inoculated with the SKOV3 cells secreting both IL-21 and GM-CSF in comparison with the nude mice inoculated with the other different SKOV3 cells. We concluded that the SKOV3 cells genetically engineered to secrete biologically active IL-21 and GM-CSF elicited antitumor immunity effectively through enhancing NK cytotoxicity, promoting the expressions of MIC A/B , ICAM-1 and NKG2D molecules as well as elevating level of IFN-gamma and TNF-alpha in the nude mice model.
机译:开发了单独分泌IL-21或与GM-CSF细胞因子组合分泌的卵巢癌细胞(SKOV3),并在裸鼠中评估了其抗肿瘤作用。通过PCR从质粒pRSC-IL-21中扩增出IL-21的基因,克隆到质粒pRSC-GM-CSF中,构建了质粒pRSC-GM-CSF-IL21。将pRSC-GM-CSF,pRSC-IL21,pRSC-GM-CSF-IL21和pRSC质粒分别转染到SKOV3细胞中,并通过分泌IL-21或与GM-CSF组合评估SKOV3细胞诱导的抗肿瘤作用。调查肿瘤的生长和裸鼠的生存。结果表明,分泌的IL-21和GM-CSF是有功能的,因为用质粒pRSC-GM-CSF-IL21转染的SKOV3细胞的培养上清液在体外增强了NK细胞毒性。 MIC A / B,NKG2D和ICAM-1分子在SKOV3细胞上的表达上调。与分别注射了IL-21和GM-CSF的SKOV3细胞一起接种的无效小鼠相比,与其他接种不同的裸鼠相比,IFN-γ和TNF-α的水平,NK细胞毒性和抗肿瘤功效显着提高。 SKOV3细胞。我们的结论是,经过基因工程改造以分泌具有生物活性的IL-21和GM-CSF的SKOV3细胞通过增强NK细胞毒性,促进MIC A / B,ICAM-1和NKG2D分子的表达以及提高IFN的水平,有效地引发了抗肿瘤免疫。 -γ和TNF-α在裸鼠模型中。

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