Issue 28, 2024

Lipo-polymeric nano-complexes for dermal delivery of a model protein

Abstract

Delivering macromolecules across the skin poses challenges due to the barrier properties of stratum corneum. Different strategies have been reported to cross this barrier, such as chemical penetration enhancers and physical methods like microneedles, sonophoresis, electroporation, laser ablation, etc. Herein, we explored a cationic lipo-polymeric nanocarrier to deliver a model protein across the skin. A cationic amphiphilic lipo-polymer was used to prepare blank nanoplexes, which were subsequently complexed with anionic fluorescein-tagged bovine serum albumin (FITC-BSA). Blank nanoplexes and FITC-BSA complexed nanoplexes showed sizes of 93.72 ± 5.8 (PDI-0.250) and 145.9 ± 3.2 nm (PDI-0.258), respectively, and zeta potentials of 25.6 ± 7.0 mV and 9.17 ± 1.20 mV. In vitro cell culture, and toxicity studies showed optimal use of these nanocarriers, with hemocompatibility data indicating non-toxicity. Ex vivo skin permeation analysis showed a skin permeation rate of 33% after 24 h. The optimized formulation was loaded in a carbopol-based gel that exhibits non-Newtonian flow characteristics with shear-thinning behavior and variable thixotropy. The nanoplexes delivered via gel demonstrated skin permeation of 57% after 24 h in mice skin ex vivo. In vivo skin toxicity testing confirmed the low toxicity profile of these nanocarriers. These results are promising for the transdermal/dermal delivery of macromolecules, such as protein therapeutics, using nanoplexes.

Graphical abstract: Lipo-polymeric nano-complexes for dermal delivery of a model protein

Supplementary files

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Article information

Article type
Paper
Submitted
27 Mar 2024
Accepted
23 May 2024
First published
26 Jun 2024
This article is Open Access
Creative Commons BY-NC license

RSC Adv., 2024,14, 20351-20364

Lipo-polymeric nano-complexes for dermal delivery of a model protein

A. Tharmatt, D. K. Sahel, R. Jatyan, A. Kumari, A. Mishra, A. Mittal and D. Chitkara, RSC Adv., 2024, 14, 20351 DOI: 10.1039/D4RA02337D

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