The Impact of Vehicle Occlusivity on Skin Delivery and Activity of a Janus Kinase Inhibitor: Comparison of Oil-Based Formulations
Paulo Sarango-Granda, Roya Mohammadi-Meyabadi, Antonio J. Braza, Lilian Sosa, Joaquim Suñer-Carbó, Mireia Mallandrich, Ana Cristina Calpena

TL;DR
This study compares oil-based formulations of a JAK inhibitor to improve topical delivery and reduce side effects in psoriasis treatment.
Contribution
The study demonstrates how vehicle occlusivity affects the stability and efficacy of topical JAK inhibitor formulations.
Findings
30% petrolatum formulations remained stable for 60 days, while higher concentrations did not.
LLV formulation showed better spreadability, sustained drug release, and higher skin retention compared to LSV.
Both formulations reduced psoriasis symptoms in vivo, confirming their anti-inflammatory efficacy.
Abstract
Background/Objectives: Baricitinib, a selective JAK1/JAK2 inhibitor, shows therapeutic potential in psoriasis; however, its oral use is associated with systemic adverse effects, encouraging the development of topical formulations. This study aimed at evaluating the influence of petrolatum type on the stability, biopharmaceutical performance, and therapeutic activity of lipid-based formulations containing Baricitinib. Methods: Formulations were prepared with Labrafac® Lipophile WL 1349 (L) and either liquid (LLV) or solid (LSV) petrolatum at 30% and 60% w/w. Stability, rheology, spreadability, in vitro release, ex vivo permeation, and skin retention were evaluated, along with the safety and efficacy in HET-CAM and imiquimod-induced psoriasis murine models. Results: Only 30% petrolatum formulations remained stable for 60 days. LLV exhibited Newtonian flow, higher spreadability, sustained…
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Taxonomy
TopicsAdvancements in Transdermal Drug Delivery · Psoriasis: Treatment and Pathogenesis · Dermatology and Skin Diseases
