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通过湿法制粒、干法制粒或直接压片法制备的亲水性基质的多模态表征方法。

Multimodal approach to characterization of hydrophilic matrices manufactured by wet and dry granulation or direct compression methods.

作者信息

Kulinowski Piotr, Woyna-Orlewicz Krzysztof, Obrał Jadwiga, Rappen Gerd-Martin, Haznar-Garbacz Dorota, Węglarz Władysław P, Jachowicz Renata, Wyszogrodzka Gabriela, Klaja Jolanta, Dorożyński Przemysław P

机构信息

Institute of Technology, The Pedagogical University of Cracow, ul. Podchorążych 2, 30-084 Kraków, Poland.

Department of Pharmaceutical Technology and Biopharmaceutics, Pharmaceutical Faculty, Jagiellonian University, ul. Medyczna 9, 30-688 Kraków, Poland.

出版信息

Int J Pharm. 2016 Feb 29;499(1-2):263-270. doi: 10.1016/j.ijpharm.2015.12.067. Epub 2016 Jan 2.

Abstract

PURPOSE OF THE RESEARCH

The purpose of the research was to investigate the effect of the manufacturing process of the controlled release hydrophilic matrix tablets on their hydration behavior, internal structure and drug release. Direct compression (DC) quetiapine hemifumarate matrices and matrices made of powders obtained by dry granulation (DG) and high shear wet granulation (HS) were prepared. They had the same quantitative composition and they were evaluated using X-ray microtomography, magnetic resonance imaging and biorelevant stress test dissolution.

PRINCIPAL RESULTS

Principal results concerned matrices after 2 h of hydration: (i) layered structure of the DC and DG hydrated tablets with magnetic resonance image intensity decreasing towards the center of the matrix was observed, while in HS matrices layer of lower intensity appeared in the middle of hydrated part; (ii) the DC and DG tablets retained their core and consequently exhibited higher resistance to the physiological stresses during simulation of small intestinal passage than HS formulation.

MAJOR CONCLUSIONS

Comparing to DC, HS granulation changed properties of the matrix in terms of hydration pattern and resistance to stress in biorelevant dissolution apparatus. Dry granulation did not change these properties-similar hydration pattern and dissolution in biorelevant conditions were observed for DC and DG matrices.

摘要

研究目的

本研究旨在考察控释亲水基质片的制备工艺对其水化行为、内部结构及药物释放的影响。制备了直接压片(DC)的半富马酸喹硫平基质片,以及通过干法制粒(DG)和高剪切湿法制粒(HS)得到的粉末制成的基质片。它们具有相同的定量组成,并采用X射线显微断层扫描、磁共振成像和生物相关应力试验溶出法进行评价。

主要结果

主要结果涉及水化2小时后的基质片:(i)观察到DC和DG水化片具有分层结构,磁共振图像强度向基质中心降低,而在HS基质片中,较低强度的层出现在水化部分的中间;(ii)DC和DG片保留了其核心,因此在模拟小肠通过过程中比HS制剂表现出更高的抗生理应力能力。

主要结论

与DC相比,HS制粒在水化模式和生物相关溶出装置中的抗应力性方面改变了基质的性质。干法制粒未改变这些性质——DC和DG基质片在生物相关条件下观察到相似的水化模式和溶出情况。

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