Topical administration of dual siRNAs using fusogenic lipid nanoparticles for treating psoriatic-like plaques

Author:

Marepally Srujan1,Boakye Cedar HA1,Patel Apurva R1,Godugu Chandraiah1,Doddapaneni Ravi1,Desai Pinaki R2,Singh Mandip1

Affiliation:

1. College of Pharmacy & Pharmaceutical Sciences, Florida A&M University, Tallahassee, FL 32307, USA.

2. Aveva Drug Delivery Systems, Miramar, FL 33025, USA

Abstract

Aim: Psoriasis is a chronic autoimmune skin disorder with substantial negative impact on the patient’s quality of life. The present study was carried out to demonstrate the efficiency of a novel topical delivery system in the transport of two siRNAs for the treatment of psoriatic-like plaques. Materials & methods: We designed and developed a novel fusogenic nucleic acid lipid particle (F-NALP) system containing two therapeutic nucleic acids, anti-STAT3 siRNA (siSTAT3) and anti-TNF-α siRNA (siTNF-α). Novel cationic amphiphilic lipid with oleyl chains was synthesized and used in the nanocarrier system. Therapeutic efficacies of F-NALPs were assessed using an imiquimod-induced psoriatic-like plaque model. Results: Hydrodynamic size and surface potential of F-NALPs were 102 ± 6 nm and 32.14 ± 6.21 mV, respectively. F-NALPs delivered fluorescein isothiocyanate-siRNA to a skin depth of 360 µm. F-NALPs carrying siSTAT3 and siTNF-α significantly (p < 0.05) reduced expression of STAT3 and TNF-α mRNAs and IL-23 and Ki-67 proteins compared with solution, and was superior in comparison with Topgraf® (GlaxoSmithKline Pharmaceuticals Limited, Maharashtra, India). Conclusion: Our observations demonstrate that F-NALPs can efficiently carry siSTAT3 and siTNF-α into the dermis and combination of the two nucleic acids can synergistically treat psoriatic-like plaques. Original submitted 5 June 2013; Revised submitted 14 October 2013

Publisher

Future Medicine Ltd

Subject

Development,General Materials Science,Biomedical Engineering,Medicine (miscellaneous),Bioengineering

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