Acceleration of in vitro dissolution studies of sustained release dosage form of theophylline and in vitro–in vivo evaluations in terms of correlations

Ertan, Gökhan; Karasulu, Ercüment; Özgüney, Işık; Karasulu, H. Yeşim; Apaydın, Şebnem; Kantarcı, Gülten; Yurdasiper, Aysu; Ege, Mehmet Ali

doi:10.1007/s13318-011-0049-6

Cited by 2 publications

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References 18 publications

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“…The principle of using accelerated testing to hasten drug release has also been successfully applied to the real-time dissolution behavior of oral controlled release tablets, resulting in a substantial reduction of analysis time in a QC setting (40)(41)(42). From these studies, it is evident that the effectiveness of an accelerated release methodology as a QC tool can be assessed by determining the robustness and discriminatory power of the procedure with respect to the in vitro release for a given product.…”

Section: Introductionmentioning

confidence: 99%

A Short Term Quality Control Tool for Biodegradable Microspheres

et al. 2014

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Accelerated in vitro release testing methodology has been developed as an indicator of product performance to be used as a discriminatory quality control (QC) technique for the release of clinical and commercial batches of biodegradable microspheres. While product performance of biodegradable microspheres can be verified by in vivo and/or in vitro experiments, such evaluation can be particularly challenging because of slow polymer degradation, resulting in extended study times, labor, and expense. Three batches of Leuprolide poly(lactic-co-glycolic acid) (PLGA) microspheres having varying morphology (process variants having different particle size and specific surface area) were manufactured by the solvent extraction/evaporation technique. Tests involving in vitro release, polymer degradation and hydration of the microspheres were performed on the three batches at 55°C. In vitro peptide release at 55°C was analyzed using a previously derived modification of the Weibull function termed the modified Weibull equation (MWE). Experimental observations and data analysis confirm excellent reproducibility studies within and between batches of the microsphere formulations demonstrating the predictability of the accelerated experiments at 55°C. The accelerated test method was also successfully able to distinguish the in vitro product performance between the three batches having varying morphology (process variants), indicating that it is a suitable QC tool to discriminate product or process variants in clinical or commercial batches of microspheres. Additionally, data analysis utilized the MWE to further quantify the differences obtained from the accelerated in vitro product performance test between process variants, thereby enhancing the discriminatory power of the accelerated methodology at 55°C.

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Section: Introductionmentioning

confidence: 99%