HPMC- and PLGA-Based Nanoparticles for the Mucoadhesive Delivery of Sitagliptin: Optimization and In Vivo Evaluation in Rats

Anroop B Nair; Nagaraja Sreeharsha; Bandar E Al-Dhubiab; Jagadeesh G Hiremath; Pottathil Shinu; Mahesh Attimarad; Katharigatta N Venugopala; Mohamed Mutahar

doi:10.3390/ma12244239

HPMC- and PLGA-Based Nanoparticles for the Mucoadhesive Delivery of Sitagliptin: Optimization and In Vivo Evaluation in Rats

Materials (Basel). 2019 Dec 17;12(24):4239. doi: 10.3390/ma12244239.

Authors

Anroop B Nair¹, Nagaraja Sreeharsha¹, Bandar E Al-Dhubiab¹, Jagadeesh G Hiremath², Pottathil Shinu³, Mahesh Attimarad¹, Katharigatta N Venugopala^{1

4}, Mohamed Mutahar⁵

Affiliations

¹ Department of Pharmaceutical Sciences, College of Clinical Pharmacy, King Faisal University, Al-Ahsa 31982, Saudi Arabia.
² Department of Pharmaceutics, PA College of Pharmacy, Mangalore 574153, Karnataka, India.
³ Department of Biomedical Sciences, College of Clinical Pharmacy, King Faisal University, Al-Ahsa 31982, Saudi Arabia.
⁴ Department of Biotechnology and Food Technology, Durban University of Technology, Durban 4000, Natal, South Africa.
⁵ Nova College of Pharmaceutical Education and Research, Jafferguda, Hayat Nagar (Mandal), Telangana 501512, India.

Abstract

Mucoadhesive nanoparticles represent a potential drug delivery strategy to enhance the therapeutic efficacy in oral therapy. This study assessed the prospective of developing HPMC- and PLGA-based nanoparticles using a nanospray drier as a mucoadhesive extended release drug delivery system for sitagliptin and evaluated their potential in an animal model. Nanoparticles were prepared using a Buchi^® B-90 nanospray drier. Optimization of particle size was performed using response surface methodology by examining the influence of spray-drying process variables (inlet temperature, feed flow, and polymer concentration) on the particle size. The prepared nanoparticles were characterized for various physicochemical characteristics (yield, drug content, morphology, particle size, thermal, and crystallographic properties) and assessed for drug release, stability, and mucoadhesive efficacy by ex vivo and in vivo studies in rats. A linear model was suggested by the design of the experiments to be the best fit for the generated design and values. The yield was 77 ± 4%, and the drug content was 90.5 ± 3.5%. Prepared nanoparticles showed an average particle size of 448.8 nm, with a narrow particle size distribution, and were wrinkled. Thermal and crystallographic characteristics showed that the drug present in the nanoparticles is in amorphous dispersion. Nanoparticles exhibited a biphasic drug release with an initial rapid release (24.9 ± 2.7% at 30 min) and a prolonged release (98.9 ± 1.8% up to 12 h). The ex vivo mucoadhesive studies confirmed the adherence of nanoparticles in stomach mucosa for a long period. Histopathological assessment showed that the formulation is safe for oral drug delivery. Nanoparticles showed a significantly higher (p < 0.05) amount of sitagliptin retention in the GIT (gastrointestinal tract) as compared to control. The data observed in this study indicate that the prepared mucoadhesive nanoparticles can be an effective alternative delivery system for the oral therapy of sitagliptin.

Keywords: drug release; mucoadhesive; nanoparticles; spray dryer.

Grants and funding

186175/Deanship of Scientific Research, King Faisal University