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首页> 外文期刊>Cancer gene therapy >SV40 Pseudovirion gene delivery of a toxin to treat human adenocarcinomas in mice
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SV40 Pseudovirion gene delivery of a toxin to treat human adenocarcinomas in mice

机译:SV40伪病毒基因基因传递毒素治疗小鼠人腺癌

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摘要

SV40 vectors packaged in vitro (pseudovirions) are an efficient delivery system for plasmids up to 17.7kb, with or without SV40 sequences. A truncated Pseudomonas exotoxin gene (PE38) was delivered into various human cells (HeLa, KB-3-1, human lymphoblastoids, and erythroleukemia cells), in vitro using pseudovirions. The number of viable cells was reduced significantly in the PE38-transduced cells. Human KB adenocarcinomas growing in mice were treated with intratumoral injection of PE38 packaged in vitro, and tumor size decreased significantly. Intraperitoneal treatments were as effective in reducing tumor size as intratumoral treatments. To check the viability of mock- or PE38-treated mice, every 4 days they were weighed, their blood was tested, and various tissues were screened for pathology. All parameters showed that the in vitro-packaged vectors, injected into tumors or intraperitoneally, caused no abnormalities in mice. The combined treatment of doxorubicin with in vitro-packaged PE38 reduced tumor size slightly more than each of the treatments separately. However, the combined treatment did not cause the weight loss seen with doxorubicin alone. These results indicate that SV40 in vitro packaging is an effective system for cancer gene delivery using two different routes of injection and in combination with chemotherapy.
机译:体外包装的SV40载体(假病毒颗粒)是一种有效的递送系统,可用于高达17.7kb的质粒(带有或不带有SV40序列)。使用假病毒颗粒在体外将截短的假单胞菌外毒素基因(PE38)递送到各种人类细胞(HeLa,KB-3-1,人类淋巴母细胞和红白血病细胞)中。在PE38转导的细胞中,活细胞的数量显着减少。用瘤内注射PE38体外包装治疗在小鼠中生长的人KB腺癌,肿瘤大小明显减少。腹膜内治疗与减少肿瘤内治疗一样有效。为了检查经模拟或PE38处理的小鼠的生存力,每隔4天称重一次,对其血液进行测试,并对各种组织进行病理筛查。所有参数均表明,注射入肿瘤或腹膜内的体外包装载体在小鼠中未引起异常。阿霉素与体外包装的PE38的联合治疗比单独的每种治疗减少的肿瘤大小稍大。但是,联合治疗并没有引起单独使用阿霉素所引起的体重减轻。这些结果表明,SV40体外包装是使用两种不同的注射途径并结合化学疗法来递送癌症基因的有效系统。

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