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一种新型万古霉素类似物的重新配方:缓冲剂种类和强度重要性的一个实例。

Reformulation of a new vancomycin analog: An example of the importance of buffer species and strength.

作者信息

Johnson Jennifer L H, Yalkowsky Samuel H

机构信息

Pharmaceutical Science, College of Pharmacy, University of Arizona, 1703 E Mabel St, 85721, Tucson, AZ.

出版信息

AAPS PharmSciTech. 2006 Mar;7(1):E33-E37. doi: 10.1208/pt070105. Epub 2017 Mar 8.

DOI:10.1208/pt070105
PMID:28290020
Abstract

The purpose of this research was to use our previously validated dynamic injection apparatus as a rapid method for screening pH-adjusted formulations of a new vancomycin analog, Van-An, for their potential to precipitate upon dilution. In 1 vial, Van-An was reconstituted according to the manufacturer's instructions. In a separate vial, the Van-An formulation's existing phosphate buffer species was supplemented with acetate buffer, which has a pKa in the desired range: between the pH values of the formulation (pH 3.9) and blood (pH 7.4). The formulations were injected using the dynamic injection apparatus into a flowing stream of isotonic Sorensen's phosphate buffer at rates of 0.25, 0.5, 1, and 2 mL/min. The peaks obtained with the spectrophotometer were reproducible for each injection rate/formulation combination. For the phosphate-buffered formulation, the least amount of precipitation was obtained at the 0.25 mL/min injection rate. Acetate buffer was able to substantially reduce such precipitation, even at the highest injection rate. The opacity peaks for the formulation with the acetate addition were significantly smaller (P<.05) than those obtained for the unaltered formulation at all 4 injection rates. The results suggest that acetate is a better buffer species than phosphate for the pH range defined. Furthermore, we present evidence to support a generally applicable approach to screening new formulations of drug products that may be clinically useful for reducing the incidence of phlebitis in humans.

摘要

本研究的目的是使用我们之前经验证的动态注射装置,作为一种快速方法来筛选新的万古霉素类似物Van - An的pH调节制剂在稀释时沉淀的可能性。在一个小瓶中,按照制造商的说明复溶Van - An。在另一个单独的小瓶中,向Van - An制剂现有的磷酸盐缓冲液中添加醋酸盐缓冲液,其pKa在所需范围内:介于制剂的pH值(pH 3.9)和血液的pH值(pH 7.4)之间。使用动态注射装置以0.25、0.5、1和2 mL/分钟的速率将制剂注入等渗的索伦森磷酸盐缓冲液的流动流中。对于每种注射速率/制剂组合,用分光光度计获得的峰是可重现的。对于磷酸盐缓冲制剂,在0.25 mL/分钟的注射速率下获得的沉淀量最少。即使在最高注射速率下,醋酸盐缓冲液也能够显著减少这种沉淀。在所有4种注射速率下,添加醋酸盐的制剂的浊度峰均明显小于未改变制剂的浊度峰(P<0.05)。结果表明,在规定的pH范围内,醋酸盐是比磷酸盐更好的缓冲液。此外,我们提供证据支持一种普遍适用的方法,用于筛选可能对降低人类静脉炎发生率具有临床实用性的药品新制剂。

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