首页> 外文期刊>Bulletin of Faculty of Pharmacy, Cairo University >Dissolution enhancement of leflunomide incorporating self emulsifying drug delivery systems and liquisolid concepts
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Dissolution enhancement of leflunomide incorporating self emulsifying drug delivery systems and liquisolid concepts

机译:结合自乳化药物递送系统和液固概念增强来氟米特的溶出度

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The objective of this study is to enhance the dissolution properties of leflunomide, a class BCS-II drug by incorporating the self emulsifying (SE) form of the drug onto liquisolid systems in the form of tablets. Different formulae were prepared by dissolving leflunomide in PEG300 then forming SE systems using tween 80 as surfactant and either sesame oil and paraffin oil then adsorbing on powder excipients to form SE liquisolid powders. The prepared powders showed adequate flowability. The drug and excipients showed compatibility by analysis with DSC, XRD and FTIR. After compression, all tablets showed adequate weight variation, friability and disintegration time with disintegration time ranging between 8.45 ± 0.16 min and 10.7 ± 0.29 min. All liquisolid tablets exhibited higher in vitro dissolution in distilled water compared to physical mixture and the commercial tablets (Arthfree?) with formula containing sesame oil and highest amount of solvent (TS04) exhibiting the highest dissolution profile and it did not change by the change in the pH of the dissolution medium. The tablets showed stability during a 6 months accelerated stability study according to appearance, drug content, disintegration time and dissolution profile. Thus it can be concluded that combining self emulsifying drug delivery technique and liquisolid technology can be a promising tool to enhance the dissolution profile of leflunomide in vitro.
机译:这项研究的目的是通过将药物的自乳化(SE)形式掺入片剂形式的液固系统中,以增强来氟米特(一种BCS-II类药物)的溶出性能。通过将来氟米特溶解在PEG300中,然后使用吐温80作为表面活性剂以及芝麻油和石蜡油形成SE系统,然后吸附在粉末赋形剂上形成SE液体固体粉末,从而制得不同的配方。制备的粉末显示出足够的流动性。通过与DSC,XRD和FTIR的分析,该药物和赋形剂显示出相容性。压片后,所有片剂均显示出足够的重量变化,易碎性和崩解时间,崩解时间介于8.45±0.16分钟和10.7±0.29分钟之间。与物理混合物相比,所有液体固体片剂在蒸馏水中的体外溶出度都更高,配方中包含芝麻油和最高溶剂量的商品片剂(Arthfree?)(TS04)的溶出度最高,并且在改变时不会改变。溶解介质的pH。根据外观,药物含量,崩解时间和溶出度,片剂在6个月加速稳定性研究中显示出稳定性。因此可以得出结论,将自乳化药物递送技术和液固技术相结合可以成为增强来氟米特体外溶出度的有前途的工具。

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