Dual release and molecular mechanism of bilayered aceclofenac tablet using polymer mixture

Hien Van Nguyen; Van Hong Nguyen; Beom-Jin Lee

doi:10.1016/j.ijpharm.2016.10.021

Dual release and molecular mechanism of bilayered aceclofenac tablet using polymer mixture

Int J Pharm. 2016 Dec 30;515(1-2):233-244. doi: 10.1016/j.ijpharm.2016.10.021. Epub 2016 Oct 12.

Authors

Hien Van Nguyen¹, Van Hong Nguyen¹, Beom-Jin Lee²

Affiliations

¹ College of Pharmacy, Ajou University, Suwon 16499, Republic of Korea.
² College of Pharmacy, Ajou University, Suwon 16499, Republic of Korea; Institute of Pharmaceutical Science and Technology, Ajou University, Suwon 16499, Republic of Korea. Electronic address: bjl@ajou.ac.kr.

PMID: 27744034
DOI: 10.1016/j.ijpharm.2016.10.021

Abstract

The objectives of the present study were to develop a controlled-release bilayered tablet of aceclofenac (AFN) 200mg with dual release and to gain a mechanistic understanding of the enhanced sustained release capability achieved by utilizing a binary mixture of the sustained release materials. Different formulations of the sustained-release layer were formulated by employing hydroxypropyl methylcellulose (HPMC) and hydroxypropyl cellulose (HPC) as the major retarding polymers. The in vitro dissolution studies of AFN bilayered tablets were carried out in intestinal fluid (pH 6.8 buffer). The mechanism of the synergistic rate-retarding effect of the polymer mixture containing HPC and carbomer was elucidated by the rate of swelling and erosion in intestinal fluid and the molecular interactions in the polymer network. The optimized bilayered tablets had similar in vitro dissolution profiles to the marketed tablet Clanza^®CR based on the similarity factor (f2) in combination with their satisfactory micromeritic, physicochemical properties, and stability profiles. Drug release from HPMC-based matrix was controlled by non-Fickian transport, while drug release from HPC-based matrix was solely governed by drug diffusion. The swelling and erosion data exhibited a dramatic increase of water uptake and a reduction of weight loss in the polymer mixture-loaded tablet. Fourier transform infrared (FTIR) spectra revealed strong hydrogen bonding between HPC and carbomer in the polymer mixture. Regarding spatial distribution of polymers in the polymer mixture-loaded tablet, carbomer was found to be the main component of the gel layer during the first 2h of the hydration process, which was responsible for retarding drug release at initial stage. This process was then followed by a gradual transition of HPC from the glassy core to the gel layer for further increasing gel strength.

Keywords: Aceclofenac; Bilayered tablet; Dual release; Mechanistic understanding; Polymer mixture; Spatial distribution of polymers; Swelling and erosion.

MeSH terms

Acrylic Resins / chemistry
Cellulose / analogs & derivatives
Cellulose / chemistry
Chemistry, Pharmaceutical / methods
Delayed-Action Preparations / chemistry
Diclofenac / analogs & derivatives*
Diclofenac / chemistry
Drug Liberation
Hypromellose Derivatives / chemistry
Polymers / chemistry*
Solubility
Tablets / chemistry*
Water / chemistry

Substances

Acrylic Resins
Delayed-Action Preparations
Polymers
Tablets
carbomer
Water
Diclofenac
Hypromellose Derivatives
Cellulose
hydroxypropylcellulose
aceclofenac