Press-Coated Aceclofenac Tablets for Pulsatile Drug Delivery: Formulation and In Vitro Evaluations.

Meshal Alshamrani,Rizwana Rashid,Muhammad Hammad Butt,Ahmad Salawi,Mahmood Ahmad,Yosif Almoshari,Muhammad Zaman,Rai Muhammad Sarfraz,Mahtab Ahmad Khan

doi:10.3390/ph15030326

Meshal Alshamrani, Rizwana Rashid + Show 7 more

Open Access

https://doi.org/10.3390/ph15030326

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Abstract

The symptoms of some diseases show circadian rhythms, such as the morning stiffness associated with pain at the time of awakening in rheumatoid arthritis. Therapy for such diseases doesn’t require immediate release or sustained release of medicament. In such therapies, pulsatile drug release is more suitable with a programmed drug release. The purpose of this research was to formulate press-coated aceclofenac tablets for pulsatile drug delivery with a distinct delay time of no drug release and release of the drug when it is more likely desired (i.e., after 5 to 6 h). Immediate release core tablets having aceclofenac were formulated. Three formulations, F1, F2, and F3, were prepared with variable concentrations of sodium croscarmellose. Pre- and post-compression tests were performed on the core tablets. The selection criteria included the lowest disintegration time as a requirement of pulsatile drug delivery with an immediate release core and a delayed release coat. The disintegration times of F1, F2, and F3 were 120 s, 60 s, and 15 s, respectively. Therefore, the F3 formulation was selected as the core tablet formulation because it had the shortest disintegration time (15 s). The core tablets were press-coated using different polymers, such as HPMC K100M, Eudragit L100, HEC, and HPMC E5. The polymers were used in the coatings to hinder the release of the core for the desired time. 36 formulations of polymer were prepared: A1 to A10 had HPMC K100M and Avicel PH102; formulations B1 to B6 had HPMC K100M, Eudragit L100, and Avicel PH102; formulations C1 to C7 had HPMC K100M and hydroxyethyl cellulose; formulations D1 to D7 had HPMC K100M and HPMC E5; and formulations E1 to E6 had changed the coating weight of the formulation used for D6 (having HPMC K100M and HPMC E5 in the ratio of 12.5% to 87.5%). Evaluations of the press-coated tablets were carried out through thickness, hardness, weight variation, friability, and in vitro dissolution tests. These parameters concluded that the formulation of E6, having HPMC K100M and HPMC E5 in the ratio of 12.5% to 87.5% at 600 mg weight, was the most optimum formulation as it showed 3.5% drug release after 4 h, 21.4% drug release after 5 h, and 99.27% drug release after 6 h.

Highlights

For specific treatments, a pulsatile drug release design displays significant advantages, where the active drug releases after a very much characterized lag time
The spectrum of FTIR of the formulation showed all the bands that were visible in the spectrum of the pure drug aceclofenac, which confirmed that the drug was compatible with the other components of the formulation, and it was not degraded by the process of forming the tablets
This was indicative of the aspect that no chemical reaction had occurred between aceclofenac and the other excipients, which was as desired

Summary

Introduction

A pulsatile drug release design displays significant advantages, where the active drug releases after a very much characterized lag time. Pharmaceuticals 2022, 15, 326 numerous illness conditions, there exists a rhythmic and temporal pattern. As numerous disease states show circadian patterns, benefits could be gained by adjusting the timing of active drug release and, likewise, the administration of medications. The formulation of a drug in such a dosage system that is administered at sleep time, with a personalized start of active drug release in the beginning hours of the morning, can provide a more beneficial treatment compared to the average sustained-release delivery system, given that more reasonable drugs are administered [2]. A pulsatile discharge framework is described as a quick and complete active drug discharge after a lag time. Along with morning stiffness at awakening, is a diagnostic characteristic of rheumatoid arthritis, and such conditions of clinical circadian manifestations are probably the result of the abnormal working of the hypothalamus

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