AUTHOR=Bednarczyk-Cwynar Barbara , Wachowiak Natalia , Szulc Michal , Kamińska Ewa , Bogacz Anna , Bartkowiak-Wieczorek Joanna , Zaprutko Lucjusz , Mikolajczak Przemyslaw L. 

TITLE=Strong and Long-Lasting Antinociceptive and Anti-inflammatory Conjugate of Naturally Occurring Oleanolic Acid and Aspirin

JOURNAL=Frontiers in Pharmacology

VOLUME=7

YEAR=2016

URL=https://www.frontiersin.org/journals/pharmacology/articles/10.3389/fphar.2016.00202

DOI=10.3389/fphar.2016.00202

ISSN=1663-9812

ABSTRACT=<p>The conjugate <bold>8</bold> was obtained as a result of condensation of 3-hydroxyiminooleanolic acid morfolide <bold>(7)</bold> and aspirin in dioxane. Analgesic effect of OAO-ASA <bold>(8)</bold> for the range of doses 0.3–300.0 mg/kg (<italic>p.o</italic>.) was performed in mice using a <italic>hot-plate</italic> test. Anti-inflammatory activity was assessed on carrageenan-induced paw edema in rats for the same range of doses. The conjugate OAO-ASA <bold>(8)</bold> did not significantly change locomotor activity of mice, therefore sedative properties of the compound should be excluded. The compound <bold>8</bold> proved a simple, proportional, dose-dependent analgesic action and expressed strong anti-inflammatory activity showing a reversed U-shaped, dose-dependent relation with its maximum at 30.0 mg/kg. After its combined administration with morphine (MF, 5.0 mg/kg, <italic>s.c</italic>.) the lowering of antinociceptive activity was found; however, the interaction with naloxone (NL, 3.0 mg/kg, <italic>s.c</italic>.) did not affect the antinociceptive effect of OAO-ASA <bold>(8)</bold>, therefore its opioid mechanism of action should be rather excluded. After combined administration with acetylsalicylic acid (ASA, 300.0 mg/kg, <italic>p.o.</italic>) in <italic>hot-plate</italic> test, the examined compound <bold>8</bold> enhanced the antinociceptive activity in significant way. It also shows that rather the whole molecule is responsible for the antinociceptive and anti-inflammatory effect of the tested compound <bold>8</bold>, however, it cannot be excluded that the summarizing effect is produced by ASA released from the compound <bold>8</bold> and the rest of triterpene derivative. The occurrence of tolerance for triterpenic derivative <bold>8</bold> was not observed, since the analgesic and anti-inflammatory effects after chronic administration of the conjugate OAO-ASA <bold>(8)</bold> was on the same level as after its single treatment. It seemed that the anti-inflammatory mechanism of action of OAO-ASA <bold>(8)</bold> is not simple, even its chronic administration lowered both blood concentration of IL-6 and mRNA IL-6 expression. However, the effects of the conjugate OAO-ASA <bold>(8)</bold> on TNF-α level and mRNA expression were opposite. Moreover, compound <bold>8</bold> did not change unequivocally mRNA TLR1, and TLR3 expression. Concluding, the obtained results regarding the antinociceptive and anti-inflammatory activity of new conjugate of oleanolic acid oxime and acetylsalicylic acid (OAO-ASA <bold>8</bold>) are very interesting, but for explanation of its mechanism of action, more detailed studies are necessary.</p>