Modern orvostudományi diagnosztikus eljárások és terápiák fejlesztése transzlációs
megközelítésbe...(EFOP-3.6.2-16-2017-00006) Funder: EFOP
(GINOP-2.3.2-15-2016-00048—STAY ALIVE)
(ÚNKP-20-5-SZTE-163)
Bólyai János Research Grant(BO/00866/20/5)
(PD129114) Funder: NRDIO
(K119938)
Subjects:
Gastroenterology and hepatology
MEDICAL AND HEALTH SCIENCES
Opioids are widely used for the pain management of acute pancreatitis (AP), but their
impact on disease progression is unclear. Therefore, our aim was to study the effects
of clinically relevant opioids on the severity of experimental AP. Various doses of
fentanyl, morphine, or buprenorphine were administered as pre- and/or post-treatments
in rats. Necrotizing AP was induced by the intraperitoneal injection of L-ornithine-HCl
or intra-ductal injection of Na-taurocholate, while intraperitoneal caerulein administration
caused edematous AP. Disease severity was determined by laboratory and histological
measurements. Mu opioid receptor (MOR) expression and function was assessed in control
and AP animals. MOR was expressed in both the pancreas and brain. The pancreatic expression
and function of MOR were reduced in AP. Fentanyl post-treatment reduced necrotizing
AP severity, whereas pre-treatment exacerbated it. Fentanyl did not affect the outcome
of edematous AP. Morphine decreased vacuolization in edematous AP, while buprenorphine
pre-treatment increased pancreatic edema during AP. The overall effects of morphine
on disease severity were negligible. In conclusion, the type, dosing, administration
route, and timing of opioid treatment can influence the effects of opioids on AP severity.
Fentanyl post-treatment proved to be beneficial in AP. Clinical studies are needed
to determine which opioids are best in AP.
