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Human Neural Stem Cells Overexpressing a Carboxylesterase Inhibit Bladder Tumor Growth

机译:人类神经干细胞过表达羧基酯酶抑制膀胱肿瘤的生长

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Bladder cancer is a significant clinical and economic problem. Despite intravesical chemotherapy and immunotherapy, up to 80% of patients with non-muscle-invasive bladder cancer develop recurrent tumors, of which 20% to 30% evolve into more aggressive, potentially lethal tumors. Recently, bladder cancer cells are considered to be mediators of resistance to current therapies and therefore represent strong candidates as biologic targets. No effective chemotherapy has yet been developed for advanced bladder cancer. It is desirable that a drug can be delivered directly and specifically to bladder cancer cells. Stem cells have selective migration ability toward cancer cells, and therapeutic genes can be easily transduced into stem cells. In suicide gene therapy for cancer, stem cells carry a gene encoding a carboxylesterase (CE) enzyme that transforms an inert CPT-11 prodrug into a toxic SN-38 product, a topoisomerase 1 inhibitor. In immunodeficient mice, systemically transplanted HB1.F3. CE stem cells migrated toward the tumor implanted by the TCCSUP bladder cancer cell line, and, in combination with CPT-11, the volume of tumors was significantly reduced. These findings may contribute to the development of a new selective chemotherapeutic strategy against bladder cancer. (C) 2016 AACR.
机译:膀胱癌是重要的临床和经济问题。尽管进行了膀胱内化学疗法和免疫疗法,但高达80%的非肌肉浸润性膀胱癌患者仍会复发,其中20%至30%会发展为更具侵略性且可能致命的肿瘤。近来,膀胱癌细胞被认为是对当前疗法的抗性的介质,因此代表了作为生物学靶标的强候选物。对于晚期膀胱癌,尚未开发出有效的化学疗法。期望可以将药物直接且特异性地递送至膀胱癌细胞。干细胞具有向癌细胞的选择性迁移能力,并且治疗基因可以轻松地转导到干细胞中。在用于癌症的自杀基因治疗中,干细胞携带一个编码羧酸酯酶(CE)酶的基因,该酶将惰性CPT-11前药转变为有毒的SN-38产品,即拓扑异构酶1抑制剂。在免疫缺陷小鼠中,系统移植了HB1.F3。 CE干细胞向由TCCSUP膀胱癌细胞系植入的肿瘤迁移,并与CPT-11结合显着减少了肿瘤的体积。这些发现可能有助于开发针对膀胱癌的新的选择性化学治疗策略。 (C)2016 AACR。

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