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首页> 外文期刊>Cancer gene therapy >Pharmacokinetics of oncolytic measles virotherapy: eventual equilibrium between virus and tumor in an ovarian cancer xenograft model
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Pharmacokinetics of oncolytic measles virotherapy: eventual equilibrium between virus and tumor in an ovarian cancer xenograft model

机译:溶瘤性麻疹病毒疗法的药代动力学:卵巢癌异种移植模型中病毒与肿瘤之间的最终平衡

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Because of their ability to replicate, the dose–response relationships of oncolytic viruses cannot easily be predicted. To better understand the pharmacokinetics of virotherapy in relation to viral dose and schedule, we administered MV-CEA intraperitoneally in an orthotopic mouse model of ovarian cancer. MV-CEA is an attenuated oncolytic measles virus engineered to express soluble human carcinoembryonic antigen (CEA), and the virus is currently undergoing phase I clinical testing in patients with ovarian cancer. Plasma CEA levels correlate with numbers of virus-infected tumor cells at a given time, and were used as a surrogate to monitor the profiles of viral gene expression over time. The antineoplastic activity of single- or multiple-dose MV-CEA was apparent over a wide range of virus doses (103–108 TCID50), with little reduction in observed antitumor efficacy, even at the lowest tested dose. However, analysis of CEA profiles of treated mice was highly informative, illustrating the variability in virus kinetics at different dose levels. The highest doses of virus were associated with higher initial levels of tumor cell killing, but the final outcome of MV-CEA therapy at all dose levels was a partial equilibrium between virus and tumor, resulting in significant slowing of tumor growth and enhanced survival of the mice.
机译:由于它们具有复制能力,因此溶瘤病毒的剂量反应关系不易预测。为了更好地了解病毒治疗与病毒剂量和时间表相关的药代动力学,我们在卵巢癌的原位小鼠模型中腹膜内施用了MV-CEA。 MV-CEA是一种工程改造为表达可溶性人类癌胚抗原(CEA)的减毒溶瘤性麻疹病毒,目前该病毒正在接受卵巢癌患者的I期临床测试。血浆CEA水平与给定时间被病毒感染的肿瘤细胞的数量相关,并被用作替代指标来监测病毒基因随时间的表达情况。单剂量或多剂量MV-CEA的抗肿瘤活性在很宽的病毒剂量范围内均很明显(103-108 TCID50),即使在最低测试剂量下,观察到的抗肿瘤功效几乎没有降低。但是,对处理过的小鼠的CEA谱图的分析非常有参考价值,说明了在不同剂量水平下病毒动力学的变化。最高剂量的病毒与较高的肿瘤细胞杀伤初始水平有关,但在所有剂量水平下,MV-CEA治疗的最终结果是病毒和肿瘤之间的部分平衡,从而导致肿瘤生长显着减慢并提高了肿瘤的存活率。老鼠。

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