首页> 外文期刊>International Journal of Pharmaceutics >Parallel screening approach to identify solubility-enhancing formulations for improved bioavailability of a poorly water-soluble compound using milligram quantities of material.
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Parallel screening approach to identify solubility-enhancing formulations for improved bioavailability of a poorly water-soluble compound using milligram quantities of material.

机译:平行筛选方法使用毫克量的材料鉴定水溶性增强的制剂,以改善水溶性差的化合物的生物利用度。

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In this article, we present a parallel experimentation approach to rapidly identify a solubility-enhancing formulation that improved the bioavailability of a poorly water-soluble compound using milligrams of material. The lead compound and a panel of excipients were dissolved in n-propanol and dispensed into the wells of a 96-well microtiter plate by a TECAN robot. Following solvent evaporation, the neat formulations were diluted with an aqueous buffer, and incubated for 24h. The solubilization capacity of the excipients for the compound at 24h (SC(24h)), was determined by HPLC, and compared with its solubility in the corresponding neat formulations determined by a bench-scale method. The ranking order of solubilization capacity of the five tested formulations for this compound by this microscreening assay is same as the ranking order of the compound solubility in the neat formulations. Several formulations that achieved the target aqueous solubility were identified using the screening method. One of the top formulations, an aqueous solution of the compound containing 20% Tween 80 by weight, increased the compound solubility from less than 2 microg/mL to at least 10mg/mL. In a rat pharmacokinetic (PK) study, the Tween 80 formulation achieved 26.6% of bioavailability, a significant improvement over 3.4% of bioavailability for the aqueous Methocel formulation (p<0.01). The results in the study suggest that this parallel screening assay can be potentially used to rapidly identify solubility-enhancing formulations for an improved bioavailability of poorly water-soluble compounds using milligram quantities of material.
机译:在本文中,我们提出了一种平行实验方法,以快速确定一种溶解度提高的配方,该配方使用毫克的材料改善了水溶性差的化合物的生物利用度。将铅化合物和一组赋形剂溶解在正丙醇中,并通过TECAN机械手分配到96孔微量滴定板的孔中。溶剂蒸发后,将纯制剂用水性缓冲液稀释,并温育24小时。通过HPLC测定赋形剂对化合物在24小时(SC(24h))的增溶能力,并与它在台式试验法确定的相应纯制剂中的溶解度进行比较。通过该微筛选测定法,五个测试制剂对该化合物的增溶能力的排名顺序与化合物在纯制剂中的溶解度的排名顺序相同。使用筛选方法鉴定了达到目标水溶性的几种制剂。顶部制剂之一是包含20重量%吐温80的化合物的水溶液,其将化合物溶解度从小于2微克/毫升增加至至少10毫克/毫升。在大鼠药代动力学(PK)研究中,吐温80制剂的生物利用度达到26.6%,比Methocel水性制剂的3.4%的生物利用度有显着改善(p <0.01)。该研究的结果表明,这种平行筛选测定法可潜在地用于以毫克量的材料快速鉴定溶解度提高的制剂,以改善水溶性差的化合物的生物利用度。

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