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NEW INTRAVENOUS DRUG ADMINISTRATION AND BLOOD SAMPLING MODEL IN THE AWAKE RAT

机译:清醒大鼠中新的静脉药物管理和血液采样模型

摘要

There is a continuing need for increased throughput in the examination of new chemical entities (NCEs) in terms of the pharmacokinetic (PK) parameters. The aim was to validate a new study method which allows a higher throughput, the examination of inter-animal variability and a reduction in the numbers of animals needed for routine bioavailability studies of NCEs in awake rats. The design uses a new method for intravenous (iv) administration via the saphenous vein in combination with serial blood sampling via the tail vein. The multiple sampling method was compared with single sampling (decapitation) and the effect on haematocrit (Hct) levels was studied. Direct injection in the saphenous vein was compared to iv administration using an indwelling jugular catheter. Using structural different CE's, it was shown that a combination of direct injection via the saphenous vein and multiple sampling from the tail vein produces comparable plasma concentrations and subsequent PK results to the comparator methods. Furthermore, Hct levels remained within recommended levels using a total blood sampling volume of up to 2.1 ml per day. The new technique increases throughput by reducing the time required for preparative surgery, increases the quality by allowing inter-animal comparison of major PK parameters as concentration time curves can be collected from each animal and reduces the number of animals required.
机译:在新的化学实体(NCE)的药代动力学(PK)参数方面,不断需要提高通量。目的是验证一种新的研究方法,该方法可以提高通量,检查动物间变异性并减少清醒大鼠NCE常规生物利用度研究所需的动物数量。该设计采用了一种通过隐静脉静脉内(iv)给药和通过尾静脉进行连续血液采样相结合的新方法。将多次取样方法与一次取样(断头)进行比较,并研究其对血细胞比容(Hct)水平的影响。使用留置颈静脉导管将隐静脉中的直接注射与静脉内注射进行比较。使用结构不同的CE,显示出通过隐静脉直接注射和从尾静脉多次采样相结合产生的血浆浓度相当,随后的PK结果可与比较方法相比。此外,使用每天最多2.1毫升的总血液采样量,Hct水平保持在推荐水平内。这项新技术通过减少准备手术所需的时间来提高产量,通过允许对主要PK参数进行动物间比较来提高质量,因为可以从每只动物收集浓度时间曲线,并减少了所需的动物数量。

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