Article date: September 2018
By: Hannah Ceuleers, Nikita Hanning, Jelena Heirbaut, Samuel Van Remoortel, Jurgen Joossens, Pieter Van Der Veken, Sven M Francque, Michelle De bruyn, Anne‐Marie Lambeir, Joris G De Man, Jean‐Pierre Timmermans, Koen Augustyns, Ingrid De Meester, Benedicte Y De Winter in Volume 175, Issue 17, pages 3516-3533
Background and Purpose
Serine proteases have been re suggested as important mediators of visceral pain. We investigated their effect by using newly developed serine protease inhibitors with a well‐characterized inhibitory profile in a rat model of post‐inflammatory irritable bowel syndrome (IBS).
Experimental Approach
Colitis was induced in rats receiving intrarectal trinitrobenzenesulphonic acid; controls received 0.9% NaCl. Colonoscopies were performed on day 3, to confirm colitis, and later until mucosal healing. Visceral hypersensitivity was quantified by visceromotor responses (VMRs) to colorectal distension, 30 min after i.p. injection of the serine protease inhibitors nafamostat, UAMC‐00050 or UAMC‐01162. Serine proteases, protease‐activated receptors (PARs) and TRP channels were quantified by qPCR and immunohistochemistry. Proteolytic activity was characterized using fluorogenic substrates.
Key Results
VMR was significantly elevated in post‐colitis rats. Nafamostat normalized VMRs at the lowest dose tested. UAMC‐00050 and UAMC‐01162 significantly decreased VMR dose‐dependently. Expression of mRNA for tryptase‐αβ‐1and PAR4, and tryptase immunoreactivity was significantly increased in the colon of post‐colitis animals. Trypsin‐like activity was also significantly increased in the colon but not in the faeces. PAR2 and TRPA1 immunoreactivity co‐localized with CGRP‐positive nerve fibres in control and post‐colitis animals.
Conclusions and Implications
Increased expression of serine proteases and activity together with increased expression of downstream molecules at the colonic and DRG level and in CGRP‐positive sensory nerve fibres imply a role for serine proteases in post‐inflammatory visceral hypersensitivity. Our results support further investigation of serine protease inhibitors as an interesting treatment strategy for IBS‐related visceral pain.
DOI: 10.1111/bph.14396
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