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Targeted therapy via oral administration of attenuated Salmonella expression plasmid-vectored Stat3-shRNA cures orthotopically transplanted mouse HCC

机译:靶向治疗通过口服施用减毒的沙门氏菌表达质粒 - 矢量化的Stat3-shRNA治疗原位移植的小鼠HCC

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摘要

The development of RNA interference-based cancer gene therapies has been delayed due to the lack of effective tumor-targeting delivery systems. Attenuated Salmonella enterica serovar Typhimurium (S. Typhimurium) has a natural tropism for solid tumors. We report here the use of attenuated S. Typhimurium as a vector to deliver shRNA directly into tumor cells. Constitutively activated signal transducer and activator of transcription 3 (Stat3) is a key transcription factor involved in both hepatocellular carcinoma (HCC) growth and metastasis. In this study, attenuated S. Typhimurium was capable of delivering shRNA-expressing vectors to the targeted cancer cells and inducing RNA interference in vivo. More importantly, a single oral dose of attenuated S. Typhimurium carrying shRNA-expressing vectors targeting Stat3 induced remarkably delayed and reduced HCC (in 70% of mice). Cancer in these cured mice did not recur over 2 years following treatment. These data demonstrated that RNA interference combined with Salmonella as a delivery system may offer a novel clinical approach for cancer gene therapy.
机译:由于缺乏有效的肿瘤靶向输送系统,RNA干扰的癌症基因疗法的发展已被延迟。减毒的沙门氏菌肠道血鼠伤寒伤寒毒蕈(S. Typhimurium)具有固体肿瘤的天然热衷。我们在此报告使用减毒的S. Typhimurium作为载体,以直接将shRNA递送到肿瘤细胞中。组成型激活的信号传感器和转录3(STAT3)的激活剂是肝细胞癌(HCC)生长和转移的关键转录因子。在该研究中,减毒的S.Typhimurium能够将表达ShRNA的载体递送到靶向癌细胞并诱导体内RNA干扰。更重要的是,携带ShRNA的诱导的诱导STRNA的诱导的诱导STRNA的诱导的STRNA的诱导的诱导的HCC(70%的小鼠中的诱导的诱导STRNA的诱导的STVIMURIUM。在治疗后,这些固化小鼠中的癌症在2年内没有复发。这些数据表明,作为递送系统的RNA干扰与沙门氏菌相结合,可以为癌症基因治疗提供新的临床方法。

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