Development and Evaluation of an Orodispersible Tablet Formation for the Delivery of a Hydrophobic Drug.

IF 2.1 Q3 PHARMACOLOGY & PHARMACY Advances in Pharmacological and Pharmaceutical Sciences Pub Date : 2024-10-17 eCollection Date: 2024-01-01 DOI:10.1155/2024/7914860

Razan Haddad, Ahmed R Gardouh

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Abstract

Orodispersible tablet (ODT) is a promising avenue for drug delivery, offering a dosage form that can be disintegrated instantaneously in the mouth and released the drug that dissolves or disperses in the saliva without the addition of water. ODT can effectively boost the dissolution rate and consequently the bioavailability of several hydrophobic drugs. Additionally, ODT is very attractive and suitable for specific patients who are unable to swallow the traditional tablet. The basic approach in the fabrication of oral tablets for hydrophobic drugs relies on the utilization of superdisintegrants which allow prompt disintegration of tablets after swallowing. In the present investigation, escitalopram oxalate was chosen as a model drug, which is a hydrophobic, antidepressant, selective serotonin reuptake inhibitor (SSRI) drug. Nine formulas of escitalopram oxalate ODTs were prepared by varying the concentrations of three different superdisintegrants: sodium starch glycolate, croscarmellose sodium, and crospovidone to improve the dissolution and release of escitalopram oxalate. Each was used in three different concentrations (2.5%, 5%, and 7.5%), and all the ODTs were prepared by the direct compression method. The micrometric characterization of the powder blend used in the formulations was investigated such as angle of repose, bulk and tapped densities, compressibility percent (Carr's index), and Hausner ratio. Furthermore, the prepared ODTs were characterized in terms of weight variation, thickness, diameter, hardness, friability, in vitro disintegration, wetting time, water absorption ratio, drug content, in vitro dissolution, and accelerated stability study. The results showed that the formula (ODT9) that contained 7.5% of the superdisintegrant sodium starch glycolate had superior characteristics in almost all the tests, with a dissolution rate of 100% after 6 minutes. Also, it was stable under the accelerated stability conditions.

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开发和评估用于输送疏水性药物的含水片剂。

口腔崩解片（ODT）是一种前景广阔的给药途径，它提供了一种可在口腔中瞬间崩解的剂型，无需加水即可将药物溶解或分散在唾液中释放出来。ODT 可以有效提高溶解率，从而提高多种疏水性药物的生物利用度。此外，对于无法吞咽传统片剂的特定患者来说，口服片剂也非常具有吸引力和适用性。制造疏水性药物口服片剂的基本方法是使用超级崩解剂，使片剂在吞咽后迅速崩解。在本次研究中，草酸艾司西酞普兰被选为一种疏水性抗抑郁选择性血清素再摄取抑制剂（SSRI）药物。为了改善草酸艾司西酞普兰的溶解和释放，我们通过改变淀粉羟乙酸钠、氨甲环酸钠和氯磺丙维酮这三种不同超微崩解剂的浓度，制备了九种草酸艾司西酞普兰 ODT 配方。每种药物都有三种不同的浓度（2.5%、5% 和 7.5%），所有 ODT 均采用直接压片法制备。研究了制剂中使用的混合粉末的微观特性，如休止角、体积密度和敲击密度、可压缩性百分比（卡尔指数）和豪斯纳比率。此外，还从重量变化、厚度、直径、硬度、易碎性、体外崩解、润湿时间、吸水率、药物含量、体外溶解和加速稳定性研究等方面对制备的 ODT 进行了表征。结果表明，含有 7.5% 超崩解剂淀粉羟乙酸钠的配方（ODT9）在几乎所有测试中都具有优异的特性，6 分钟后的溶解率为 100%。此外，它在加速稳定性条件下也很稳定。

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