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Adenovirus-mediated FasL gene transfer into human gastric carcinoma

机译:腺病毒介导的FasL基因转移至人胃癌

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evaluate the possible value of FasL in gastric cancer gene therapy by investigating the effects of FasL expression on human gastric cancer cell line.An adenoviral vector encoding the full-length human FasL cDNA was constructed and used to infect a human gastric cancer (SGC-7901) cell line. FasL expression was confirmed by X-gal staining, flow cytometric analysis and RT-PCR. The effect of FasL on cell proliferation was determined by clonogenic assay, cytotoxicity was detected by MTT assay, and cell viability was measured by trypan blue exclusion. The therapeutic efficiency of Ad-FasL in vivo was investigated with a xenograft tumor model in nude mice.SGC-7901 cells infected with Ad-FasL showed increased expression of FasL, resulting in significantly decreased cell growth and colony-forming activity when compared with control adenovirus-infected cells. The cytotoxicity of anti-Fas antibody (CH-11) in gastric cancer cells was stronger than that of ActD (91±8 vs 60±5, P<0.01), and the cytotoxicity of Ad-FasL was stronger than that of CH-11 (60±5 vs 50±2, P<0.05). In addition, G1-phase arrest (67.75±0.39 vs58.03±2.16, P<0.05) and apoptosis were observed in Ad-FasL-infected SGC-7901 cells, and the growth of SGC-7901 xenografts in nude mice was retarded after intra-tumoral injection with Ad-FasL (54% vs 0%, P<0.0001).Infection of human gastric carcinoma cells with Ad-FasL induces apoptosis, indicating that this target gene might be of potential value in gene therapy for gastric cancer.
机译:通过研究FasL表达对人胃癌细胞系的影响,评估FasL在胃癌基因治疗中的可能价值。构建了编码全长人FasL cDNA的腺病毒载体,并将其用于感染人胃癌(SGC-7901 )细胞系。通过X-gal染色,流式细胞术分析和RT-PCR证实FasL表达。通过克隆形成测定确定FasL对细胞增殖的作用,通过MTT测定检测细胞毒性,并且通过锥虫蓝排除法测量细胞活力。用异种移植瘤模型在裸鼠中研究了Ad-FasL的体内治疗效果。感染Ad-FasL的SGC-7901细胞显示FasL表达增加,与对照相比明显降低了细胞生长和集落形成活性腺病毒感染的细胞。抗Fas抗体(CH-11)在胃癌细胞中的细胞毒性强于ActD(91±8 vs 60±5,P <0.01),而Ad-FasL的细胞毒性强于CH-。 11(60±5 vs 50±2,P <0.05)。此外,感染Ad-FasL的SGC-7901细胞观察到G1期阻滞(67.75±0.39 vs 58.03±2.16,P <0.05)和凋亡,且SGC-7901异种移植后裸鼠的生长受到抑制肿瘤内注射Ad-FasL(54%vs 0%,P <0.0001)。Ad-FasL感染人胃癌细胞会诱导细胞凋亡,表明该靶基因可能在胃癌基因治疗中具有潜在价值。

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