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粉末溶解测量的微型化和粒度估计。

Miniaturization of powder dissolution measurement and estimation of particle size.

机构信息

pION Inc., 5 Constitution Way, Woburn, MA 01801, USA.

出版信息

Chem Biodivers. 2009 Nov;6(11):1796-811. doi: 10.1002/cbdv.200900082.

Abstract

The objective was to investigate the applicability and limitations of an approach for estimating particle size from powder dissolution measurement using as little as 50 microg of sample in 1 ml of buffer solutions. The powder dissolution profiles of five sparingly-soluble drugs (hydrochlorothiazide, phenazopyridine hydrochloride, 2-naphthoic acid, indomethacin, and dipyridamole) were evaluated with a novel biexponential spherical particle equation and also the Wang-Flanagan spherical particle non-sink equation. The results were compared to particle sizing based on measured specific surface area by the Brunauer-Emmett-Teller (BET) method, and also based on Coulter counting. With the exception of hydrochlorothiazide, the model compounds indicated some agglomeration in the dissolution media. The dry-state specific surface area was larger than expected from either the Coulter method or the powder-dissolution data, especially for phenazopyridine hydrochloride. The particle radii estimated by the powder dissolution method ranged from 10 to 68 microm, with equilibrium solubilities spanning from 5 microg/ml (dipyridamole) to 911 microg/ml (hydrochlorothiazide). Powder dissolution data collected with the miniaturized apparatus can be used to determine particle size, with estimated values agreeing reasonably with those measured by the Coulter counter method.

摘要

目的在于研究一种方法的适用性和局限性,该方法通过在 1 毫升缓冲溶液中使用少至 50 微克的样品来从粉末溶解测量中估算粒度。使用新型双指数球形颗粒方程和 Wang-Flanagan 球形颗粒非溶出方程评估了五种难溶性药物(氢氯噻嗪、盐酸phenazopyridine、2-萘酸、吲哚美辛和双嘧达莫)的粉末溶解曲线。将结果与通过 Brunauer-Emmett-Teller(BET)法测量的比表面积、库尔特计数法的粒径进行比较。除了氢氯噻嗪之外,模型化合物在溶解介质中显示出一些团聚。干燥状态下的比表面积大于库尔特法或粉末溶解数据的预期值,尤其是对于盐酸phenazopyridine。通过粉末溶解法估算的粒径范围为 10 至 68 微米,平衡溶解度从 5 微克/毫升(双嘧达莫)到 911 微克/毫升(氢氯噻嗪)。使用微型化装置收集的粉末溶解数据可用于确定粒径,估算值与库尔特计数器法测量的值相当吻合。

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