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Efficacy of recombinant adenoviral human p53 gene in the treatment of lung cancer-mediated pleural effusion

机译:重组腺病毒人p53基因在肺癌介导的胸腔积液治疗中的功效

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Pleural effusion induced by lung cancer exerts a negative impact on quality of life and prognosis. The aim of the present study was to evaluate the value of the recombinant adenoviral human p53 gene (rAd-p53) in the local treatment of lung cancer and its synergistic effect with chemotherapy. The present study retrospectively recruited 210 patients with lung cancer-mediated pleural effusion who had adopted a treatment strategy of platinum chemotherapy. Pleurodesis was performed via the injection of cisplatin or rAd-p53. Long-term follow-up was conducted to investigate the therapeutic effects of cisplatin and rAd-p53 administration on pleural effusion and other relevant clinical indicators. The short-term effect of pleurodesis was as follows: The efficacy rate of rAd-p53 therapy was significantly higher compared with cisplatin therapy (71.26 vs. 54.47%), and the efficacy of treatment with >= 2x10(12) viral particles of rAd-p53 for pleurodesis was significantly greater than treatment with 40 mg cisplatin (P<0.05). Furthermore, efficacy analysis performed 6 and 12 months after pleurodesis indicated that the efficacy rate of rAd-p53 was significantly greater than that of cisplatin (P<0.05). A comparison of median progression-free survival (PFS) time identified a significant difference (P<0.05) between rAd-p53 and cisplatin therapy (3.3 vs. 2.7 months); however, a comparison of median overall survival time identified no significant difference (P>0.05) between rAd-p53 and cisplatin therapy (9.6 vs. 8.7 months). In addition, Cox regression analysis indicated that PFS was not affected by clinical indicators such as age, gender, prognostic staging and smoking status; however, PFS was affected by pathological subtype (adenocarcinoma or squamous carcinoma) in the rAd-p53 group. rAd-p53 administration for pleurodesis exerts long-term therapeutic effects on the local treatment of lung cancer. Thus, a combination of rAd-p53 and chemotherapy may exert a synergistic effect and reverse multidrug resistance.
机译:肺癌引起的胸腔积液对生活质量和预后产生负面影响。本研究的目的是评估重组腺病毒人p53基因(rAd-p53)在肺癌局部治疗中的价值及其与化疗的协同作用。本研究回顾性研究了210例采用铂类化疗策略的肺癌介导的胸腔积液患者。通过注射顺铂或rAd-p53进行胸膜固定术。进行了长期随访,以研究顺铂和rAd-p53给药对胸腔积液及其他相关临床指标的治疗作用。胸膜固定术的短期疗效如下:rAd-p53疗法的疗效显着高于顺铂疗法(71.26 vs. 54.47%),以及> = 2x10(12)的rAd病毒颗粒疗法的疗效-p53用于胸膜固定术的疗效显着高于40 mg顺铂治疗(P <0.05)。此外,在胸膜固定术后6和12个月进行的功效分析表明,rAd-p53的功效显着高于顺铂(P <0.05)。通过比较中位无进展生存时间(PFS),可以确定rAd-p53与顺铂治疗之间存在显着差异(P <0.05)(3.3 vs. 2.7个月)。然而,对中位总生存时间的比较发现,rAd-p53和顺铂治疗之间无显着差异(P> 0.05)(9.6个月与8.7个月)。此外,Cox回归分析表明,PFS不受年龄,性别,预后分期和吸烟状况等临床指标的影响。然而,rAd-p53组的PFS受病理亚型(腺癌或鳞状癌)的影响。使用rAd-p53进行胸膜固定术对肺癌的局部治疗具有长期治疗作用。因此,rAd-p53和化学疗法的组合可能发挥协同作用,并逆转多药耐药性。

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