基于 Kollidon®SR 的二元控释基质片剂的崩解行为:不同理化性质和压实性质的药物或辅料的影响研究

IF 3.4 4区 医学 Q2 PHARMACOLOGY & PHARMACY
Wasfy M. Obeidat, Shadi F. F. Gharaibeh
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引用次数: 0

摘要

本研究的目的是考察负载药物或赋形剂的理化特性、Kollidon®SR(KSR)的浓度以及 KSR 压片的机械特性对其崩解时间的影响。使用崩解仪器,选择两小时作为过程的终点。压缩压力最高的乳糖-KSR 密实物和 KSR 浓度超过 30% 的微晶纤维素-KSR 密实物的崩解时间均少于十分钟。同样,在所有测试的 KSR 浓度和压缩压力下,含有盐酸地尔硫卓-KSR 的压制物的崩解时间都很短。含有莫达非尼、盐酸二甲双胍和抗坏血酸-KSR 的复方制剂的崩解时间从快速到适中不等,取决于所使用的 KSR 浓度和压缩压力。含有阿司匹林、水杨酸或布洛芬的 KSR 复方片,即使 KSR 含量极低(0.5%),也不会出现明显的崩解。茶碱-KSR 片也显示出较长的崩解时间,即使 KSR 的浓度很低。Dic-KSR 药片的崩解时间大致接近一小时,主要不受不同 KSR 含量的影响,仅受压缩压力的轻微影响。由此可以得出结论,不同的药物或辅料对抵抗压片崩解过程的最低 KSR 要求不同。在水中溶解度低的化合物可能会导致 KSR 压片崩解时间延长。这些化合物的熔点与压制物的 Py 值及其压制特性结合在一起,可能会影响崩解过程,不过还需要进行精确的评估。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Investigations on the Impacts of Drugs or Excipients with Different Physicochemical and Compaction Properties on the Disintegration Behavior of Kollidon®SR-Based Binary Controlled Release Matrix Tablets

Investigations on the Impacts of Drugs or Excipients with Different Physicochemical and Compaction Properties on the Disintegration Behavior of Kollidon®SR-Based Binary Controlled Release Matrix Tablets

The objective of this study was to examine the impact of the physicochemical properties of the loaded drug or excipient, the concentration of Kollidon®SR (KSR), and the mechanical characteristics of KSR compacts on their disintegration times. Using disintegration apparatus, a two-hour constraint was chosen as the process's end point. Lactose-KSR compacts subjected to the highest compression pressure and Microcrystalline cellulose-KSR compacts with KSR concentrations exceeding 30% exhibited disintegration times of less than ten minutes. Likewise, compacts containing Diltiazem HCl-KSR demonstrated brief disintegration times across all tested KSR concentrations and compression pressures. Compacts of Modafinil, Metformin HCl, and Ascorbic acid-KSR displayed disintegration times ranging from fast to moderate, contingent upon the levels of KSR and compression pressure applied. Compacts containing KSR with Aspirin, Salicylic acid, or Ibuprofen did not exhibit significant disintegration even at minimal amounts of KSR (0.5%). Theophylline-KSR tablets also showed prolonged dissolution times, even at very low concentrations of KSR. The disintegration times of Dic-KSR tablets were roughly close to an hour and were predominantly unaffected by varying KSR levels and only marginally influenced by compression pressures. It is possible to draw the conclusion that different drugs or excipients have different minimum KSR requirements to resist compacts’ disintegration process. Compounds that demonstrate low solubility in water can result in extended disintegration times for KSR compacts. The melting points of these compounds, in conjunction with the Py values of the compacts and their compaction properties, could affect the disintegration process, although a precise evaluation is necessary.

Graphical Abstract

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来源期刊
AAPS PharmSciTech
AAPS PharmSciTech 医学-药学
CiteScore
6.80
自引率
3.00%
发文量
264
审稿时长
2.4 months
期刊介绍: AAPS PharmSciTech is a peer-reviewed, online-only journal committed to serving those pharmaceutical scientists and engineers interested in the research, development, and evaluation of pharmaceutical dosage forms and delivery systems, including drugs derived from biotechnology and the manufacturing science pertaining to the commercialization of such dosage forms. Because of its electronic nature, AAPS PharmSciTech aspires to utilize evolving electronic technology to enable faster and diverse mechanisms of information delivery to its readership. Submission of uninvited expert reviews and research articles are welcomed.
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