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首页> 外文期刊>Journal of pharmaceutical sciences. >Correlation of tissue-plasma partition coefficients between normal tissues and subcutaneous xenografts of human tumor cell lines in mouse as a prediction tool of drug penetration in tumors
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Correlation of tissue-plasma partition coefficients between normal tissues and subcutaneous xenografts of human tumor cell lines in mouse as a prediction tool of drug penetration in tumors

机译:正常组织与人肿瘤细胞系皮下异种移植物之间的组织-血浆分配系数的相关性作为预测药物在肿瘤中渗透的工具

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Understanding drug distribution and accumulation in tumors would be informative in the assessment of efficacy in targeted therapy; however, existing methods for predicting tissue drug distribution focus on normal tissues and do not incorporate tumors. The main objective of this study was to describe the relationships between tissue-plasma concentration ratios (Kp) of normal tissues and those of subcutaneous xenograft tumors under nonsteady-state conditions, and establish regression equations that could potentially be used for the prediction of drug levels in several human tumor xenografts in mouse, based solely on a Kp value determined in a normal tissue (e.g., muscle). A dataset of 17 compounds was collected from the literature and from Genentech. Tissue and plasma concentration data in mouse were obtained following oral gavage or intraperitoneal administration. Linear regression analyses were performed between Kp values in several normal tissues (muscle, lung, liver, or brain) and those in human tumor xenografts (CL6, EBC-1, HT-29, PC3, U-87, MCF-7-neo-Her2, or BT474M1.1). The tissue-plasma ratios in normal tissues reasonably correlated with the tumor-plasma ratios in CL6, EBC-1, HT-29, U-87, BT474M1.1, and MCF-7-neo-Her2 xenografts (r2 in the range 0.62-1) but not with the PC3 xenograft. In general, muscle and lung exhibited the strongest correlation with tumor xenografts, followed by liver. Regression coefficients from brain were low, except between brain and the glioblastoma U-87 xenograft (r2 in the range 0.62-0.94). Furthermore, reasonably strong correlations were observed between muscle and lung and between muscle and liver (r2 in the range 0.67-0.96). The slopes of the regressions differed depending on the class of drug (strong vs. weak base) and type of tissue (brain vs. other tissues and tumors). Overall, this study will contribute to our understanding of tissue-plasma partition coefficients for tumors and facilitate the use of physiologically based pharmacokinetics (PBPK) modeling for chemotherapy in oncology studies.
机译:了解肿瘤中药物的分布和蓄积将有助于评估靶向治疗的疗效;然而,现有的预测组织药物分布的方法集中在正常组织上,并且没有合并肿瘤。这项研究的主要目的是描述非稳态条件下正常组织与皮下异种移植肿瘤的组织血浆浓度比(Kp)之间的关系,并建立可用于预测药物水平的回归方程。仅基于正常组织(例如,肌肉)中确定的Kp值,在小鼠的几种人类肿瘤异种移植物中检测到的“肿瘤”。从文献和Genentech收集了17种化合物的数据集。口服管饲或腹膜内给药后获得小鼠的组织和血浆浓度数据。在几种正常组织(肌肉,肺,肝或脑)和人肿瘤异种移植物(CL6,EBC-1,HT-29,PC3,U-87,MCF-7-neo)的Kp值之间进行线性回归分析-Her2或BT474M1.1)。正常组织的组织血浆比率与CL6,EBC-1,HT-29,U-87,BT474M1.1和MCF-7-neo-Her2异种移植物中的肿瘤血浆比率合理相关(r2的范围为0.62 -1),但不适用于PC3异种移植。通常,肌肉和肺与肿瘤异种移植的相关性最强,其次是肝脏。除大脑与胶质母细胞瘤U-87异种移植之间(r2在0.62-0.94范围内)外,来自大脑的回归系数很低。此外,在肌肉和肺之间以及肌肉和肝脏之间观察到相当强的相关性(r2在0.67-0.96范围内)。回归的斜率根据药物类别(强碱与弱碱)和组织类型(脑部与其他组织和肿瘤)的不同而不同。总体而言,这项研究将有助于我们了解肿瘤的组织-血浆分配系数,并有助于在肿瘤学研究中将基于生理学的药代动力学(PBPK)模型用于化学疗法。

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