Development of a Topical Treatment for Psoriasis Targeting RORγ: From Bench to Skin

<div><p>Background</p><p>Psoriasis is a chronic inflammatory skin disorder involving marked immunological changes. IL-17-targeting biologics have been successful in reducing the disease burden of psoriasis patients with moderate-to-severe disease. Unfortunately, the stratum corneum prevents penetration of large molecule weight proteins, including monoclonal antibodies. Thus, for the majority of psoriasis patients ineligible for systemic treatments, a small molecule targeting RORγt, the master regulator of IL-17 family cytokines, may represent an alternative topical medicine with biologic-like efficacy.</p><p>Methods and Findings</p><p>The preclinical studies described in this manuscript bridge the gap from bench to bedside to provide the scientific foundation for a compound entering clinical trials for patients with mild to moderate psoriasis. In addition to several ex vivo reporter assays, primary T cell cultures, and the imiquimod mouse model, we demonstrate efficacy in a newly developed human ex vivo skin assay, where Th17-skewed cytokine expression is induced from skin-resident immune cells. Importantly, the skin barrier remains intact allowing for the demonstration of topical drug delivery. With the development of this novel assay, we demonstrate potent compound activity in the target tissue: human skin. Finally, target engagement by this small molecule was confirmed in <i>ex vivo</i> lesional psoriatic skin.</p><p>Conclusions</p><p>Our work describes a progressive series of assays to demonstrate the potential clinical value of a novel RORγ inverse agonist small molecule with high potency and selectivity, which will enter clinical trials in late 2015 for psoriasis patients.</p></div

Skin Resident Immune Cell Activation (sRICA) leads to pro-inflammatory cytokine responses that are reduced by GSK2981278.

<p>(A) Skin explants were cultured ≥4 days under the indicated conditions. Explants were analyzed for tissue integrity by H&E. (B) Samples were pre-treated with 10 μM compound (closed bar) or vehicle (DMSO; open bars–set to 100%) for 1 day prior to 24–48 hrs of Th17 stimulation. Relative transcript levels were determined by qRT-PCR. (C) Samples were treated as in B, then analyzed daily for tissue integrity by H&E. Images are representative at least 3 independent experiments. (D) Samples were treated as in B. Graphs show the mean percent maximum stimulation of 3 independent experiments. Significant inhibition was determined by Student’s <i>t</i> test. (*p≤0.05; **p≤0.01; ***p≤0.001).</p

GSK2981278 attenuates inflammation in a mouse model of psoriasis.

<p>(A) Mice were treated topically with placebo or 1% GSK2981278 (1278) in ointment, and with imiquimod (IMQ) or petrolatum (vehicle). At study’s end (day +9 of IMQ treatment), back skin was imaged and stained (H&E). (B) Mean epidermal thickness is shown across 6–9 mice per treatment group. (C-E) Changes to local cytokine expression was determined following topical application of 1% or 0.1% compound in a simple ethanolic solution (60:40 ethanol:water). (C) Description of study groups for panels D-E. Skin cytokine levels on day +3 (D) or day +9 (E). Data reflect the mean ± SEM gene expression level across 6–9 mice per treatment group. Significant inhibition was determined by Student’s <i>t</i> test. (*p≤0.05;**p≤0.01).</p

Treatment of psoriatic tissue with the RORγ inverse agonist GSK2981278 reduces proinflammatory cytokine levels.

<p>Three psoriatic skin biopsies were obtained via 3-4mm punch biopsy and placed in Unisol buffer for overnight shipment. Upon arrival, biopsy sections were placed in Cornification media without stimulation for 12–14 hours with either 0.2% DMSO or 10 μM compound. The percent inhibition of each biomarker compared to culture with DMSO alone is shown. Each point represents an individual patient sample. The percent maximum expression ± SEM for each analyte assayed of each tissue was calculated relative to time zero. Significant inhibition was determined by Paired <i>t</i>-test. (**p≤0.01).</p

Suppression of Th17-type cytokine production following topical application.

<p><i>Ex vivo</i> human skin was cultured in Franz Cell chambers for a total of 48 hours. GSK2981278 was applied to the dry surface of the skin at time zero followed 24 hrs later by activation of skin resident immune cells under Th17 polarizing conditions. The experimental schema is shown in panel A. Skin sections were harvested after 24 hrs of stimulation (48 hrs of compound treatment) and analyzed for relative gene expression of <i>il17a</i> (B) or <i>il17f</i> (C). Data are shown as the percent maximum expression of each cytokine as compared to Th17-stimulated samples treated topically with vehicle only.</p

Bivalve distribution in hydrographic regions in South America: historical overview and conservation

Based on literature review and malacological collections, 168 native freshwater bivalve and five invasive species have been recorded for 52 hydrographic regions in South America. The higher species richness has been detected in the South Atlantic, Uruguay, Paraguay, and Amazon Brazilian hydrographic regions. Presence or absence data were analysed by Principal Coordinate for PhylogenyWeighted. The lineage Veneroida was more representative in hydrographic regions that are poorer in species and located West of South America. The Mycetopodidae and Hyriidae lineages were predominant in regions that are richest in species toward the East of the continent. The distribution of invasive speciesLimnoperna fortuneiis not related to species richness in different hydrographic regions there. The species richness and its distribution patterns are closely associated with the geological history of the continent. The hydrographic regions present distinct phylogenetic and species composition regardless of the level of richness. Therefore, not only should the richness be considered to be a criterion for prioritizing areas for conservation, but also the phylogenetic diversity of communities engaged in services and functional aspects relevant to ecosystem maintenance. A plan to the management of this fauna according to particular ecological characteristics and human uses of hydrographic regions is neededFil: Pereira, Daniel . Universidade Federal Do Rio Grande Do Sul; BrasilFil: Dreher Mansur, Maria Cristina . Universidade Federal Do Rio Grande Do Sul; BrasilFil: Duarte, Leandro D. S. . Universidade Federal Do Rio Grande Do Sul; BrasilFil: Schramm de Oliveira, Arthur . Universidade Federal Do Rio Grande Do Sul; BrasilFil: Mansur Pimpao, Daniel . Universidade Federal Do Rio Grande Do Sul; BrasilFil: Tasso Callil, Claudia . Universidade Federal Do Mato Grosso Do Sul; BrasilFil: Ituarte, Cristian Federico. Consejo Nacional de Investigaciones Científicas y Técnicas. Oficina de Coordinación Administrativa Parque Centenario. Museo Argentino de Ciencias Naturales; ArgentinaFil: Parada, Esperanza . Plataforma de Investigación en Ecohidrología y Ecohidráulica (ECOHYD); ChileFil: Peredo, Santiago . Plataforma de Investigación en Ecohidrología y Ecohidráulica (ECOHYD); ChileFil: Darrigran, Gustavo Alberto. Universidad Nacional de la Plata. Facultad de Cs.naturales y Museo. Div.zoologia Invertebrados; Argentina. Consejo Nacional de Investigaciones Científicas y Técnicas; ArgentinaFil: Scarabino, Fabrizio . Museo Nacional de Historia Natural; UruguayFil: Clavijo, Cristhian. Museo Nacional de Historia Natural; UruguayFil: Lara, Gladys . Universidad Católica de Temuco; ChileFil: Miyahira, Igor Christo . Universidade do Estado do Rio de Janeiro; BrasilFil: Raya Rodriguez, Maria Teresa . Universidade Federal Do Rio Grande Do Sul; BrasilFil: Lasso, Carlos . Instituto de Investigacion de Recursos Biologicos Alexander von Humboldt; Colombi