Preparation and Characterization of Stable Nanosuspension for Dissolution Rate Enhancement of Furosemide: A Quality by Design (QbD) Approach

Akbar L Marzan; Rahnuma Tabassum; Basarat Jahan; Mehedi H Asif; Hasan M Reza; Mohsin Kazi; Sultan M Alshehri; Marcel de Matas; Mohammad H Shariare

doi:10.2174/1567201815666180123094320

Preparation and Characterization of Stable Nanosuspension for Dissolution Rate Enhancement of Furosemide: A Quality by Design (QbD) Approach

Curr Drug Deliv. 2018;15(5):672-685. doi: 10.2174/1567201815666180123094320.

Authors

Akbar L Marzan¹, Rahnuma Tabassum¹, Basarat Jahan¹, Mehedi H Asif¹, Hasan M Reza¹, Mohsin Kazi², Sultan M Alshehri², Marcel de Matas³, Mohammad H Shariare¹

Affiliations

¹ Department of Pharmaceutical Sciences, North South University, Dhaka, Bangladesh.
² Department of Pharmaceutics, College of Pharmacy, King Saud University, Riyadh, Saudi Arabia.
³ SEDA Pharmaceutical Development Services, Alderley Park, Cheshire, United Kingdom.

PMID: 29359667
DOI: 10.2174/1567201815666180123094320

Abstract

Background: Nano drug delivery systems have the potential to address the challenges of delivering BCS Class II and IV drugs like furosemide. The purpose of the current study is to prepare stable nanosuspension and investigate in vitro dissolution performance of the model compound furosemide using quality by design (QbD) approach.

Methods: Nanosuspension batches with uniform particle size were prepared for furosemide using the antisolvent precipitation method. A quality by design (Qbd) approach was explored to understand the impact of process parameters (stirring time, stirring speed, temperature, and injection rate) and material attributes (drug concentration, stabilizer type, drug: stabilizer ratio, and antisolvent: solvent ratio) on the quality attributes of furosemide nanosuspension using a full factorial experimental design. Multiple linear regression and ANOVA were employed to estimate and identify the critical process parameters and material attributes. Injection rate and stirring time were identified as the most critical process parameters' affecting the quality attributes of furosemide nanosuspension.

Results: Individual material attributes did not show significant impact on the average particle size of the nanocrystals, however two-way interactions between material attributes (stabilizer type/drug concentration and stabilizer type/antisolvent: solvent ratio) significantly affected nanosuspension particle size distribution. Solid state characterization (PXRD, DSC and SEM) did not exhibit any changes of physical form during preparation and optimization of the furosemide nanosuspension. Dissolution of the furosemide nanocrystals in gastric media was significantly higher than that observed for micronized furosemide suspension and raw furosemide powder. Stability study data suggests that optimized batches of furosemide nanosuspensions were stable for three months at 4°C and ambient conditions.

Conclusion: The antisolvent precipitation method can produce stable furosemide nanosuspensions with desirable quality attributes and enhancement of dissolution rate in the gastric medium as compared to the raw furosemide powder and microsuspension.

Keywords: Antisolvent precipitation; QbD; furosemide; nano drug delivery; nanosuspension; stabilizer..

MeSH terms

Diuretics / chemistry*
Drug Design
Drug Liberation
Drug Stability
Furosemide / chemistry*
Microscopy, Electron, Scanning
Nanoparticles / chemistry*
Nanoparticles / ultrastructure
Particle Size
Suspensions

Substances

Diuretics
Suspensions
Furosemide