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Title: | Low dose of carvacrol prevents rat pancreas tissue damage after L-arginine application, while higher doses cause pancreatic tissue impairment | Authors: | Stojanović, Nikola Stevanović, Milica Ranđelović, Pavle Mitić, Katarina Petrović, Vladimir Sokolović, Dušan Mladenović, Bojan Lalić, Jelena Radulović, Niko |
Keywords: | Carvacrol;;Toxicity;;Pancreas;;L-arginineα;;a-amylase;;Lipase;;Malondialdehyde | Issue Date: | Jun-2019 | Rank: | M21a | Publisher: | Elsevier | Journal: | Food and Chemical Toxicology | Volume: | 128 | Start page: | 280 | End page: | 285 | Abstract: | Carvacrol (5-isopropyl-2-methylphenol) is a biologically active monoterpene phenol abundantly present in the essential oils of many Lamiaceae aromatic/ethnomedicinal plants. Herein, we aimed to evaluate the damaging effect of carvacrol to rat pancreatic tissue, but also to assess its possible ameliorative impact on pancreatic damage induced by L-arginine. The toxic and beneficial (in a dose of 10 mg/kg) properties of carvacrol were assessed by measuring serum α-amylase and lipase activities, tissue malondialdehyde (MDA) content, and pathohistological changes in pancreatic tissue. Application of 100/500 mg/kg of carvacrol produced a significant increase in α-amylase activity, followed by inflammatory-cell infiltration and patchy interlobular edema in the pancreas. In the L-arginine-induced pancreatitis model, a dose of 10 mg/kg of carvacrol prevented an increase in α-amylase and lipase activities, and MDA formation, when compared to the animals that received L-arginine only. Animals treated with carvacrol prior to L-arginine administration displayed mild edema and inflammatory infiltration with few necrotic areas. Contrary to that, animals that received only L-arginine showed a massive leukocyte infiltrate with edema and substantial necrotic areas. In our study carvacrol showed significant protective effects and a potential to modulate leukocyte recruitment in pancreatic tissue after L-arginine injection. |
URI: | https://biore.bio.bg.ac.rs/handle/123456789/6124 | DOI: | 10.1016/j.fct.2019.04.010 |
Appears in Collections: | Journal Article |
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