Neurotensin-based hybrid peptides anti-inflammatory activity in murine model of a contact sensitivity response.pdfVIP

Neurotensin-based hybrid peptides anti-inflammatory activity in murine model of a contact sensitivity response.pdf

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Neurotensin-based hybrid peptides anti-inflammatory activity in murine model of a contact sensitivity response.pdf

European Journal of Pharmaceutical Sciences 93 (2016) 84–89 Contents lists available at ScienceDirect European Journal of Pharmaceutical Sciences journal homepage: /locate/ejps Neurotensin-based hybrid peptides anti-in?ammatory activity in murine model of a contact sensitivity response Katarzyna Kaczyńska a,?, Ewelina Kogut a, Dominika Zaj?c a, Monika Jampolska a, Kryspin Andrzejewski a, Dorota Sulejczak b, Andrzej W. Lipkowski c, Patrycja Kleczkowska c,d a Laboratory of Respiration Physiology, Mossakowski Medical Research Centre, Polish Academy of Sciences, Warsaw, Poland b Department of Experimental Pharmacology, Mossakowski Medical Research Centre, Polish Academy of Sciences, Warsaw, Poland c Department of Neuropeptides, Mossakowski Medical Research Centre, Polish Academy of Sciences, Warsaw, Poland d Department of Pharmacodynamics, Centre for Preclinical Research and Technology, Medical University of Warsaw, Poland article info Article history: Received 11 April 2016 Received in revised form 12 July 2016 Accepted 5 August 2016 Available online 7 August 2016 Keywords: Contact sensitivity Ear swelling IL-1α MCP-1 TNF-α Hybrid peptide abstract The objective of the study was to investigate the possibility of modulation of skin in?ammation by topical treatment with a novel compound: an opioid-neurotensin hybrid peptide PK20 encompassing endomorphin-2 analog and modi?ed fragment of neurotensin (8–13). Contact sensitivity response was induced in mice by skin sensitization with dinitro?uorobenzene (DNFB) followed by topical hapten application on ears. Mice were treated locally with PK20 or pure cream 2 h after the challenge with DNFB. 2 and 24 h after hapten exposure, ear thickness was determined. Ears were collected for histology and homogenization. Supernatants were used for measurement of contents of cytokines and lipid peroxidation products. Treatment with PK20 reduced signi?cantly the late phase of contact sensitivity response, which was revealed by ear thickness d

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