首页> 外文期刊>British Journal of Cancer >Adenoviral vector-mediated expression of a gene encoding secreted, EpCAM-targeted carboxylesterase-2 sensitises colon cancer spheroids to CPT-11
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Adenoviral vector-mediated expression of a gene encoding secreted, EpCAM-targeted carboxylesterase-2 sensitises colon cancer spheroids to CPT-11

机译:腺病毒载体介导的编码分泌型,EpCAM靶向的羧酸酯酶2编码基因的表达使结肠癌球体对CPT-11敏感

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CPT-11 (irinotecan or 7-ethyl-10[4-(1-piperidino)-1-piperidino] carbonyloxycamptothecin) is an anticancer agent in use for the treatment of colon cancer. In order to be fully active, CPT-11 needs to be converted into SN-38 (7-ethyl-10-hydroxycamptothecin) by the enzyme carboxylesterase (CE). In humans, only a minority of CPT-11 is converted to SN-38. To increase the antitumour effect of CPT-11 by gene-directed enzyme prodrug therapy, we constructed a replication-deficient adenoviral vector Ad.C28-sCE2 containing a fusion gene encoding a secreted form of human liver CE2 targeted to the surface antigen epithelial cell adhesion molecule (EpCAM) that is highly expressed on most colon carcinoma cells. By targeting CE2 to EpCAM, the enzyme should accumulate specifically in tumours and leakage into the circulation should be minimised. Ad.C28-sCE2-transduced colon carcinoma cells expressed and secreted active CE that bound specifically to EpCAM-expressing cells. In sections of three-dimensional colon carcinoma spheroids transduced with Ad.C28-sCE2, it was shown that C28-sCE2 was capable of binding untransduced cells. Most importantly, treatment of these spheroids with nontoxic concentrations of CPT-11 resulted in growth inhibition comparable to treatment with SN-38. Therefore, Ad.C28-sCE2 holds promise in gene therapy approaches for the treatment of colon carcinoma.
机译:CPT-11(伊立替康或7-乙基-10 [4-(1-哌啶子基)-1-哌啶子基]羰氧基喜树碱)是用于治疗结肠癌的抗癌药。为了充分发挥活性,CPT-11需要通过羧酸酯酶(CE)转化为SN-38(7-乙基-10-羟基喜树碱)。在人类中,只有少数CPT-11被转换为SN-38。为了通过基因定向酶前药治疗提高CPT-11的抗肿瘤作用,我们构建了复制缺陷型腺病毒载体Ad.C28-sCE2,该载体包含编码靶向表面抗原上皮细胞黏附的分泌形式的人肝CE2的融合基因。在大多数结肠癌细胞中高度表达的分子(EpCAM)。通过将CE2靶向EpCAM,该酶应专门在肿瘤中蓄积,并应最大程度地减少循环中的泄漏。 Ad.C28-sCE2转导的结肠癌细胞表达并分泌了特异性结合EpCAM表达细胞的活性CE。在用Ad.C28-sCE2转导的三维结肠癌球体的切片中,表明C28-sCE2能够结合未转导的细胞。最重要的是,用无毒浓度的CPT-11处理这些球体的效果与SN-38相当。因此,Ad.C28-sCE2在基因治疗方法中有望用于治疗结肠癌。

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