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Effects of hypoxia and limited diffusion in tumor cell microenvironment on bystander effect of P450 prodrug therapy

机译:缺氧和肿瘤细胞微环境中有限扩散对P450前药治疗旁观者效应的影响

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Cytochrome P450 (CYP) enzyme 2B1 metabolizes the anticancer prodrug cyclophosphamide (CPA) to 4-hydroxy-CPA, which decomposes to the cytotoxic metabolites acrolein and phosphoramide mustard. We have evaluated the bystander cytotoxicity of CPA in combination with CYP2B1 gene-directed enzyme prodrug therapy using a cell culture-based agarose overlay technique. This method mimics the tumor microenvironment by limiting the diffusion of metabolites and by reducing the oxygen concentration to levels similar to those found in solid tumors. Under these conditions, the CYP activity of CYP2B1-expressing tumor cells was decreased by 80% compared to standard aerobic conditions. Despite this decrease in metabolic activity, a potent bystander effect was observed, resulting in up to 90% killing by CPA of a tumor cell population comprised of only 20% CYP-expressing tumor cells. Similarly, transient transfection of a small fraction (14%) of a human hepatoma Huh7 cell population with a CYP2B1 expression plasmid followed by short-term treatment with CPA (5h) led to an eradication of 95% of the cells. No such bystander effect was observed without the agarose overlay. These findings suggest that the agarose overlay technique is very useful as an in vitro test system for investigation of the bystander effect of CYP/CPA and other enzyme/prodrug combinations under conditions that mimic the hypoxic conditions present in solid tumors in vivo.
机译:细胞色素P450(CYP)酶2B1将抗癌前药环磷酰胺(CPA)代谢为4-羟基-CPA,后者分解为细胞毒性代谢产物丙烯醛和磷酰胺芥菜。我们已经评估了CPA与基于细胞培养的琼脂糖覆盖技术联合CYP2B1基因指导的酶前药治疗的旁观者细胞毒性。该方法通过限制代谢物的扩散并通过将氧浓度降低到与实体瘤相似的水平来模拟肿瘤的微环境。在这些条件下,与标准有氧条件相比,表达CYP2B1的肿瘤细胞的CYP活性降低了80%。尽管代谢活性降低,但仍观察到有效的旁观者效应,导致仅由20%CYP表达的肿瘤细胞组成的肿瘤细胞群体被CPA杀死的可能性高达90%。同样,用CYP2B1表达质粒瞬时转染一小部分(14%)人肝癌Huh7细胞群体,然后短期用CPA处理(5h),导致根除95%的细胞。没有琼脂糖覆盖,没有观察到这种旁观者效应。这些发现表明琼脂糖覆盖技术作为体外测试系统非常有用,可用于在模拟体内实体瘤中存在的低氧条件下研究CYP / CPA和其他酶/前药组合的旁观者效应。

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