Formulation of Gelled Microemulsion for Effective Permeation of Celecoxib Across the Skin Barrier

Author:

Siddique Muhammad Yasir1,Nazar Muhammad Faizan2ORCID,Saleem Muhammad Atif1,Haider Sajjad3,Sumrra Sajjad Hussain1,Akhtar Muhammad Saeed4,Farooqi} Zahoor H.5

Affiliation:

1. Department of Chemistry University of Gujrat Gujrat 50700 Pakistan

2. Department of Chemistry University of Education Lahore Multan Campus 60700 Pakistan

3. Chemical Engineering Department College of Engineering King Saud University P.O.Box 800 Riyadh 11421 Saudi Arabia

4. School of Chemical Engineering Yeungnam University Gyeongsan 38541 Republic of Korea

5. School of Chemistry University of the Punjab New Campus Lahore Pakistan

Abstract

AbstractMicroemulsion‐based gels (μEGs) are smart colloidal carriers, superior to traditional topical formulations due to formulation simplicity, structural flexibility, high stability, and controlled delivery of topical drugs through biofilms. Here, we report a new μEG formulation for topical application of an anti‐inflammatory drug, celecoxib (CXB). For this, the μE system was formulated using olive oil (~10 %), Water (~15 %), Tween‐80 (~67.5 %) and Span‐80 (~7.5 %) to enhanced the loading of CXB (~2.0 wt.%), and then gelled to semisolid μEG by the addition of polyethylene glycol 6000 (PEG‐6000) (2.0 wt.%) to modulate CXB passage across the skin‐barriers. Optical microscopy showed the transition from water‐in‐oil (w/o) to oil‐in‐water (o/w) through bicontinuous networks. Dynamic light scattering and electron micrographs demonstrate very fine unimodal assembly of CXB‐μE nanodroplets (~65 nm), which didn't amalgamate to form spherical CXB‐μEG (~95 nm) after gelation. Moreover, FTIR analysis showed effective encapsulation of CXB into hydrophobic microenvironment with no observable chemical interaction between CXB and μE excipients, which was further verified by the peak‐to‐peak measurement of fluorescence. Further, ex‐vivo permeation of CXB‐μEG showed enhanced and persistent permeation (>99 %) within 10 hours at pH=5.5 into rabbit skin barrier. This demonstrates the sustained release of CXB in μEG and the enhancement in transdermal delivery over its conventional topical formulations.

Funder

Higher Education Commision, Pakistan

King Saud University

Department of Chemistry, University of York

University of Gujrat

Publisher

Wiley

Subject

General Chemistry

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