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盐酸地尔硫䓬与聚醋酸乙烯酯(PVAc)和聚乙烯吡咯烷酮(PVP)共喷雾干燥并物理混合后制成的缓释片剂。

Sustained release of diltiazem HCl tableted after co-spray drying and physical mixing with PVAc and PVP.

作者信息

Al-Zoubi Nizar, Al-Obaidi Ghada, Tashtoush Bassam, Malamataris Stavros

机构信息

a Faculty of Pharmaceutical Sciences, Hashemite University , Zarqa , Jordan .

b Faculty of Pharmacy, Applied Science University , Amman , Jordan .

出版信息

Drug Dev Ind Pharm. 2016;42(2):270-9. doi: 10.3109/03639045.2015.1047848. Epub 2015 Jun 2.

Abstract

In this work, aqueous diltiazem HCl and polyvinyl-pyrrolidone (PVP) solutions were mixed with Kollicoat SR 30D and spray dried to microparticles of different drug:excipient ratio and PVP content. Co-spray dried products and physical mixtures of drug, Kollidon SR and PVP were tableted. Spray drying process, co-spray dried products and compressibility/compactability of co-spray dried and physical mixtures, as well as drug release and water uptake of matrix-tablets was evaluated. Simple power equation fitted drug release and water uptake (R(2) > 0.909 and 0.938, respectively) and correlations between them were examined. Co-spray dried products with PVP content lower than in physical mixtures result in slower release, while at equal PVP content (19 and 29% w/w of excipient) in similar release (f2 > 50). Increase of PVP content increases release rate and co-spray drying might be an alternative, when physical mixing is inadequate. Co-spray dried products show better compressibility/compatibility but higher stickiness to the die-wall compared to physical mixtures. SEM observations and comparison of release and swelling showed that distribution of tableted component affects only the swelling, while PVP content for both co-spray dried and physical mixes is major reason for release alterations and an aid for drug release control.

摘要

在本研究中,将盐酸地尔硫䓬水溶液和聚乙烯吡咯烷酮(PVP)溶液与Kollicoat SR 30D混合,并喷雾干燥成不同药物:辅料比例和PVP含量的微粒。将共喷雾干燥产品以及药物、Kollidon SR和PVP的物理混合物压片。对喷雾干燥过程、共喷雾干燥产品以及共喷雾干燥和物理混合物的可压缩性/成型性,以及基质片剂的药物释放和吸水性进行了评估。用简单幂方程拟合药物释放和吸水性(R²分别>0.909和0.938),并研究了它们之间的相关性。PVP含量低于物理混合物的共喷雾干燥产品导致释放较慢,而在PVP含量相等(辅料的19%和29% w/w)时释放相似(f2>50)。PVP含量的增加会提高释放速率,当物理混合不充分时,共喷雾干燥可能是一种替代方法。与物理混合物相比,共喷雾干燥产品显示出更好的可压缩性/相容性,但对模壁的粘性更高。扫描电子显微镜观察以及释放和溶胀的比较表明,压片成分的分布仅影响溶胀,而共喷雾干燥和物理混合物的PVP含量是释放改变的主要原因,也是控制药物释放的一个辅助因素。

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