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The establishment of a growth-controllable orthotopic bladder cancer model through the down-regulation of c-myc expression

机译:通过下调c-myc表达建立生长可控原位膀胱癌模型

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摘要

To properly evaluate the biological effects of immunotherapy, it is critical to utilize a model of cancer in immune-competent mice. Currently, MBT-2 is the most common murine bladder cancer cell line used in orthotopic bladder cancer models, even though this cell type often has an inappropriate genetic mutation landscape. In these models, after tumors are detected with in vivo imaging, the mouse usually dies within two to three weeks due to post-renal azotemia caused by the rapidly growing mass. This event prohibits the evaluation of tumor behavior upon intravesical drug treatment. We explored whether an shRNA-induced decrease in the expression of the c-myc oncogene in MBT-2 cells could slow down their in vitro proliferation and in vivo tumor growth. We transduced MBT-2 cells with shRNA lentiviruses that bound c-myc, established MBT2.cMYCshRNA and confirmed the retardation of the growth of tumors implanted in C3H/He mice. Accordingly, this study suggests that this novel orthotopic bladder cancer model in immune-competent mice may be more appropriate for the analysis of the effects of the intravesical instillation of immunotherapeutic agents.
机译:为了正确评估免疫疗法的生物学效应,至关重要的是在具有免疫能力的小鼠中使用癌症模型。目前,MBT-2是原位膀胱癌模型中使用的最常见的鼠类膀胱癌细胞系,即使这种细胞类型通常具有不适当的遗传突变情况。在这些模型中,通过体内成像检测到肿瘤后,小鼠通常会在两到三周内死亡,这是由于快速增长的肿块引起的肾脏后氮质血症。该事件禁止在膀胱内药物治疗后评估肿瘤行为。我们探讨了shRNA诱导的MBT-2细胞中c-myc癌基因表达的降低是否会减慢其体外增殖和体内肿瘤的生长。我们用结合c-myc的shRNA慢病毒转导了MBT-2细胞,建立了MBT2.cMYCshRNA,并证实了植入C3H / He小鼠体内的肿瘤生长受阻。因此,这项研究表明,这种具有免疫功能的小鼠的新型原位膀胱癌模型可能更适合于膀胱内滴注免疫治疗剂的影响。

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