Optimizing the IMQ model: Deep characterization of the human TLR7 response for early drug development

Author:

Noort Juliette Anne van den1,Assil Salma1,Ronner Micha Nathaniel1,Osse Michelle1,Pot Iris2,Yavuz Yalçin1,Damman Jeffrey3,Lubberts Erik3,Rissmann Robert1,Kolk Tessa Niemeyer- van der1,Tomljanovic Ingrid3,Jansen Manon Aleida Adriana1,Moerland Matthijs1

Affiliation:

1. Centre for Human Drug Research

2. Leiden Academic Centre for Drug Research

3. Erasmus University Medical Centre

Abstract

Abstract

Purpose Imiquimod (IMQ; brand name Aldara®) is a registered topical agent that has been proven to induce local inflammation via the Toll-like receptor (TLR)7 pathway. The purpose of this study was to characterize TLR7-mediated inflammation following 7 days (168h) of topical IMQ exposure in healthy volunteers, and to compare the effects of short exposure (48h-72h) with prolonged exposure (120h-168h). Methods IMQ (100mg) was applied under occlusion to 5 different tape-stripped treatment sites on the back of 10 healthy participants for a maximum of 7 consecutive days. Erythema and skin perfusion were measured daily up to 168h. Biopsies for immunohistochemical staining and RNA sequencing were collected at 0h, 48h, 72h, 120h and 168h post IMQ application. Results IMQ triggered an inflammatory response starting at 48h after application, including erythema and perfusion of the skin. At the transcriptomic level, IMQ induced TLR7 signalling, IRF involvement and activation of TNF signalling via NF-κB. Furthermore, an enhanced inflammatory response at the cellular level was observed after prolonged IMQ exposure, with cellular infiltration of dendritic cells, macrophages and T cells which was also corroborated by transcriptomic profiles. No difference was found in the erythema and perfusion response after 168h of IMQ exposure compared to 72h. Conclusion Prolonged IMQ exposure revealed enhanced cellular responses and additional pathways with modulated activity compared to short exposure and can therefore be of interest as a model for investigational compounds targeting innate and adaptive immune responses.

Publisher

Springer Science and Business Media LLC

Reference39 articles.

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