Tissue distribution and physiologically based pharmacokinetics of antisense phosphorothioate oligonucleotide ISIS 1082 in rat.

B. Peng, J. Andrews, I. Nestorov, B. Brennan, P. Nicklin, M. Rowland
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引用次数: 39

Abstract

The aim of this study was to develop a whole body physiologically based model of the pharmacokinetics (PBPK) of the phosphorothioate oligonucleotide (PS-ODN) ISIS 1082 in vivo. Rats were administered an intravenous (i.v.) bolus dose of ISIS 1082 (10 mg/kg plus 3H tracer), and arterial blood and tissues were taken at specific times up to 72 hours. Radioactivity was measured in all samples. The parent compound was determined specifically in blood and tissues at 90 minutes and in liver and kidney also at 24 hours, using capillary gel electrophoresis (CGE). A whole body PBPK model was fitted to the combined blood and tissue radioactivity data using nonlinear regression analysis. CGE analysis indicated that the predominant species in plasma and all tissues is ISIS 1082, together with some n-1 and n-2 metabolites. Total radioactivity primarily reflects these species. The whole body model successfully described temporal events in all tissues. However, to adequately model the experimental data, all tissues had to be partitioned into vascular and extravascular spaces to accommodate the relatively slow distribution of ISIS 1082 out of blood because of a permeability rate limitation. ISIS 1082 distributes extensively into tissues, but the relative affinity varies enormously, being highest for kidney and liver and lowest for muscle and brain. A whole body PBPK model with a permeability rate limited tissue distribution was developed that adequately described events in both blood and tissue for an oligonucleotide. This model has the potential not only to characterize the events in individual tissues throughout the body for such compounds but also to scale across animal species, including human.
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反义硫代寡核苷酸ISIS 1082在大鼠体内的组织分布及生理药代动力学。
本研究的目的是建立一个基于全体生理的硫代寡核苷酸(PS-ODN) ISIS 1082体内药代动力学(PBPK)模型。大鼠静脉注射ISIS 1082 (10mg /kg + 3H示踪剂),并在特定时间取动脉血液和组织至72小时。在所有样品中都测量了放射性。用毛细管凝胶电泳(CGE)测定90分钟血液和组织以及24小时肝脏和肾脏中母体化合物的特异性。采用非线性回归分析方法,对血液和组织放射性数据拟合出全身PBPK模型。CGE分析表明,在血浆和所有组织中,优势种为ISIS 1082,并伴有部分n-1和n-2代谢产物。总放射性主要反映这些物质。全身模型成功地描述了所有组织中的时间事件。然而,为了充分模拟实验数据,所有组织都必须被分割成血管和血管外空间,以适应ISIS 1082在血液中相对缓慢的分布,这是由于渗透率的限制。ISIS 1082在组织中分布广泛,但相对亲和力差异很大,对肾脏和肝脏的亲和力最高,对肌肉和大脑的亲和力最低。建立了一个渗透率有限的组织分布的全身PBPK模型,该模型充分描述了一个寡核苷酸在血液和组织中的事件。该模型不仅具有表征此类化合物在全身单个组织中发生的事件的潜力,而且还具有跨动物物种(包括人类)扩展的潜力。
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