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首页> 外文期刊>CPT: Pharmacometrics & Systems Pharmacology >Preclinical Modeling of Tumor Growth and Angiogenesis Inhibition to Describe Pazopanib Clinical Effects in Renal Cell Carcinoma
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Preclinical Modeling of Tumor Growth and Angiogenesis Inhibition to Describe Pazopanib Clinical Effects in Renal Cell Carcinoma

机译:肿瘤生长和血管生成抑制作用的临床前模型描述帕唑帕尼在肾细胞癌中的临床作用

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摘要

AbstractThe objective was to leverage tumor size data from preclinical experiments to propose a model of tumor growth and angiogenesis inhibition for the analysis of pazopanib efficacy in renal cell carcinoma (RCC) patients. We analyzed tumor data in mice with RCC CAKI-2 cell line treated with pazopanib. Clinical tumor size data obtained in a subset of patients with RCC were also analyzed. A model accounting for the processes of tumor growth, angiogenesis, and drug effect was developed. The final tumor model was composed of two variables: the tumor and its vasculature. Our results show that, both in mice and in humans, pazopanib exhibits a dual mechanism of action, and parameter estimation values highlight the inherent difference between mice and humans on the time scale of tumor size response. We developed a semimechanistic tumor growth inhibition model that takes into account tumor angiogenesis in order to describe the effects of pazopanib in mice. Analyzing rich preclinical data with a semimechanistic model may be a relevant approach to facilitate the description of sparse clinical longitudinal tumor size data and to provide insights for the understanding of the drug mechanisms of action in patients.
机译:摘要目的是利用临床前实验中的肿瘤大小数据建立一个肿瘤生长和血管生成抑制模型,以分析帕唑帕尼对肾细胞癌(RCC)患者的疗效。我们分析了用帕唑帕尼治疗的RCC CAKI-2细胞系小鼠的肿瘤数据。还分析了一部分RCC患者获得的临床肿瘤大小数据。建立了解释肿瘤生长,血管生成和药物作用过程的模型。最终的肿瘤模型由两个变量组成:肿瘤及其脉管系统。我们的结果表明,无论在小鼠还是人类中,帕唑帕尼都具有双重作用机制,参数估计值突出了小鼠和人类在肿瘤大小反应的时间尺度上的内在差异。我们开发了一种考虑肿瘤血管生成的半机械肿瘤生长抑制模型,以描述帕唑帕尼在小鼠中的作用。用半力学模型分析丰富的临床前数据可能是一种有助于简化临床纵向稀疏肿瘤大小数据描述并为理解患者药物作用机理提供见解的相关方法。

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