4.4 Article

Supernatants of irritable bowel syndrome mucosal biopsies impair human colonic smooth muscle contractility

期刊

NEUROGASTROENTEROLOGY AND MOTILITY
卷 29, 期 2, 页码 -

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WILEY
DOI: 10.1111/nmo.12928

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colonic motility; human smooth muscle; irritable bowel syndrome; mucosal supernatants

资金

  1. University Sapienza of Rome [000324_13]

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BackgroundChanges in intestinal motility are likely to contribute to irritable bowel syndrome (IBS) pathophysiology. The aim of the study was to investigate the effects of IBS mucosal supernatants on human colonic muscle contractility. MethodsSupernatants were obtained from biopsies of 18 IBS patientsnine with constipation (IBS-C) and nine with diarrhea-predominant IBS (IBS-D)and nine asymptomatic subjects, used as controls. Colonic circular smooth muscle strips or isolated cells (SMC) were exposed to control or IBS supernatants. Spontaneous phasic contractions on strips and morphofunctional parameters on cells were evaluated in basal conditions and in response to acetylcholine (Ach). Incubation with IBS supernatants was also conducted in the presence of antagonists and inhibitors (namely histamine, protease and prostaglandin antagonists, nuclear factor-kappa B inhibitor, catalase, NADPH oxidase inhibitor, and the cAMP- and/or cGMP-cyclase inhibitors). Key ResultsExposure to IBS-C and IBS-D supernatants induced a significant reduction in basal tone and Ach-elicited contraction of muscle strips and a significant shortening and impairment of Ach contraction of SMCs. The NADPH oxidase inhibitor prevented the effect of supernatants, while the protease antagonist only IBS-C effect. No effect was observed with the other antagonists and inhibitors. Dilution of IBS-D supernatants partially restored the effects only on SMCs, whereas dilution of IBS-C supernatants significantly reverted the effects on muscle strips and Ach-elicited response on SMC. Conclusions & InferencesSupernatants from mucosal biopsies of IBS patients reduce colonic contractility. The observed impairment was concentration dependent, likely occurring through intracellular oxidative stress damage, involving different neuromotor mechanisms depending on the IBS subtype.

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