Solid nanoemulsion as antigen and immunopotentiator carrier for transcutaneous immunization

6533b86ffe1ef96bd12cd39d

RESEARCH PRODUCT

Solid nanoemulsion as antigen and immunopotentiator carrier for transcutaneous immunization

Hansjörg Schild Markus P. Radsak Philipp Arnold Pamela Stein K.d. Lee Karsten Gogoll Peter Langguth Tanja Peters

subject

0301 basic medicine Skin Neoplasms Chemistry Pharmaceutical Immunology Antineoplastic Agents Imiquimod Immunopotentiator Biology Administration Cutaneous 030226 pharmacology & pharmacy Mice 03 medical and health sciences Freeze-drying Squalene chemistry.chemical_compound Drug Delivery Systems 0302 clinical medicine Adjuvants Immunologic Antigen In vivo medicine Animals Humans Active ingredient Imiquimod Chromatography Vaccination Permeation Nanostructures Mice Inbred C57BL 030104 developmental biology chemistry Langerhans Cells Immunology Aminoquinolines Immunization Oils Precancerous Conditions medicine.drug

description

Imiquimod, a toll-like receptor 7 (TLR7) agonist, is an active pharmaceutical ingredient (API) established for the topical treatment of several dermal cancerous and precancerous skin lesions. Within this work, the immunostimulatory effect of imiquimod is further exploited in a transcutaneous immunization (TCI) approach based on a solid nanoemulsion (SN) formulation. SN contains a combination of imiquimod with the model peptide antigen SIINFEKL as a novel approach to omit needle and syringe and optimize dermal antigen administration. Excipients including sucrose fatty acid esters and the pharmaceutically acceptable oils MCT (middle chain triglycerides), avocado oil, jojoba wax and squalene are high pressure homogenized together with the antigen SIINFEKL. Freeze drying was performed to eliminate water and to achieve spreadable properties of the formulation for dermal administration. The influence of the different oil components was assessed regarding in vitro drug permeation in a Franz diffusion cell model using a murine skin setup. In vivo performance in terms of cytotoxic T-cell response was assessed in a C57BL/6 mouse model. Whereas Aldara® cream contains imiquimod in a dissolved state, the SN formulations carry the active in a suspended state. This resulted in a reduction of imiquimod permeation across murine skin from the SN when compared to Aldara® cream. In spite of this permeation rate reduction, each SN induced an in vivo immune response by specific T-cell lysis. A stabilized solid nanosuspension containing squalene/tocopherol exhibited a significantly higher performance (p⩽0.05) in comparison with Aldara® cream. MCT based SN exerted an in vivo effect comparable to Aldara®. In conclusion, anhydrous highly dispersed vehicles containing imiquimod in a submicron particle size distribution can represent promising formulations for TCI. The choice of the oil component has a strong influence on SN performance, independent of in vitro drug permeation.

year	journal	country	edition	language
2015-10-26	Cellular Immunology

https://doi.org/10.1016/j.cellimm.2016.06.001