Role of nitric oxide in determination of large intestinal contractility in neonatal rats

Abstract

Nitric oxide (NO) plays a key role in inhibiting the contractility of gut smooth muscles in various species, and NG-nitro-L-arginine methyl ester (L-NAME) is a critical NO synthase inhibitor. Previous research investigating the role of NO in regulating gut motility focused on adult animals. Therefore, more research is needed to determine their status in the gut of newborns. Our study intended to understand how NO impacts the large gut contractility, in vitro, in rats, both neonates and adults, to get a better insight into the physiological role of NO in regulating large gut motility, particularly in neonates. In an organ bath preparation, the segments of a large gut (colon and rectum) were subjected to various concentrations of nitroglycerin (NG) (0.01–100 mM), a NO donor, cumulatively. In another group, pre-treatment with L-NAME (100 mM) was done to evaluate the blocking effect of NO on the contractile tension and frequency. NG induced relaxation in the colon and rectum of adult rats in a similar manner. NG caused significantly greater relaxation in neonates’ rectums than in their colons. In neonatal and adult rats, L-NAME pre-application inhibited NG-induced relaxation in contractile tension. Exposure to different concentrations of NG decreased contractile frequency in adult rats’ colons and rectum. However, L-NAME pre-treatment did not affect the decrease in contractile frequency caused by NG. In neonates, NG caused a concentration-dependent reduction in contractile frequency, and a decrease in contractile frequency in the rectum was more than that in the colon. However, L-NAME pre-treatment did not affect the reduction in contractile frequency caused by NG. Nitrergic mechanisms have possibly been present since birth. The intensity of control by NO may be different in the colon and rectum. The differences in NO sensitivity in adults and neonates demonstrated the changes during development.