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使用逆向透析和零净通量进行微透析校准:应用于齐多夫定在兔脑脊液和丘脑分布的研究

Microdialysis calibration using retrodialysis and zero-net flux: application to a study of the distribution of zidovudine to rabbit cerebrospinal fluid and thalamus.

作者信息

Wang Y, Wong S L, Sawchuk R J

机构信息

Department of Pharmaceutics, College of Pharmacy, University of Minnesota, Minneapolis 55455.

出版信息

Pharm Res. 1993 Oct;10(10):1411-9. doi: 10.1023/a:1018906821725.

Abstract

A retrodialysis (RD) method for the real-time calibration of on-line microdialysis (MD) procedures was investigated in vitro and in vivo. Calibration by retrodialysis was simultaneously validated through the use of a zero-net flux (ZNF) method, which assumes directional independence of diffusion of the solute. In RD, a calibrator with dialysance (PeA; effective permeability-surface area product) similar to that of the compound of interest is introduced into the perfusate. If the calibrator is suitable, its loss from the perfusate during RD is identical to the recovery of the solute of interest determined simultaneously by normal MD. Two antiviral nucleosides (AZT and AZdU) which differ structurally by only a methylene group were utilized as solute and calibrator, respectively. Both nucleosides exhibited similar recovery and loss at flow rates of 0.5 to 5 microL/min in vitro, indicating a similar PeA product in this flow domain. Furthermore, both compounds showed similar loss into the lateral ventricle or thalamus of rabbits (n = 4) during RD at a flow rate of 1 microL/min for 6 hr. The relative loss decreased rapidly within the first hour, reaching a relatively stable value after 2 hr. The significant reduction in the loss of AZdU and AZT in vivo compared with that in vitro likely results from a lower diffusion coefficient in tissue. The distribution of AZT between plasma and cerebrospinal fluid (CSF) in the ventricle and extracellular fluid (ECF) in thalamus was determined at steady state using calibration by RD and ZNF simultaneously.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

一种用于在线微透析(MD)程序实时校准的逆向透析(RD)方法在体外和体内进行了研究。通过使用零净通量(ZNF)方法同时验证了逆向透析校准,该方法假定溶质扩散的方向独立性。在RD中,将具有与目标化合物相似透析率(PeA;有效渗透表面积乘积)的校准物引入灌注液中。如果校准物合适,其在RD过程中从灌注液中的损失与通过正常MD同时测定的目标溶质的回收率相同。分别使用结构上仅相差一个亚甲基的两种抗病毒核苷(AZT和AZdU)作为溶质和校准物。在体外流速为0.5至5微升/分钟时,两种核苷均表现出相似的回收率和损失率,表明在该流速范围内具有相似的PeA乘积。此外,在1微升/分钟的流速下进行6小时的RD期间,两种化合物在兔(n = 4)的侧脑室或丘脑中的损失相似。相对损失在第一小时内迅速下降,2小时后达到相对稳定的值。与体外相比,AZdU和AZT在体内损失的显著降低可能是由于组织中较低的扩散系数。使用RD和ZNF校准同时在稳态下测定了AZT在脑室血浆与脑脊液(CSF)以及丘脑中细胞外液(ECF)之间的分布。(摘要截断于250字)

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