Lyophilised aqueous extract of Euphorbia hirta L. (Euphorbiaceae) has been evaluated for analgesic, antipyretic and anti-inflammatory properties in mice and rats, in order to complete its activity profile, after the confirmation of the existence of a central depressant activity particularly expressed by a strong sedative effect, associated with anxiolytic effects. This study leads us to the conclusion that this plant extract exerts central analgesic properties. Such a dose-dependent action was obtained against chemical (writhing test) and thermic (hot plate test) stimuli, respectively, from the doses of 20 and 25 mg/kg and it was inhibited by a naloxone pretreatment, a specific morphinic antagonist compound. An antipyretic activity was obtained at the sedative doses of 100 and 400 mg/kg, on the yeast-induced hyperthermia. Finally, significant and dose-dependent anti-inflammatory effects were observed on an acute inflammatory process (carrageenan-induced edema test in rats) from the dose of 100 mg/kg. On the other hand, plant extract remained inactive on chronic processes such as Freund's adjuvant-induced rheumatoid arthritis, after a chronic treatment during fourteen days at the daily dose of 200 or 400 mg/kg; however, if inefficacy was observed on rat backpaws edema and on loss of weight, the aqueous extract reduced the inflammatory hyperalgia.
Tert-butyl hydroperoxide induces in freshly isolated rat hepatocytes malonaldehyde formation and lacticodehydrogenase and aspartate amino-transferase leakage. This model, when adapted to crude extracts, permits the demonstration of both anti-lipoperoxidant and antihepatotoxic activity of reference products like quercetin and silymarin and plant extracts like Rosmarinus officinalis and Eschscholzia californica.
A lyophilized aqueous extract of Euphorbia hirta L. (Eh) has been evaluated for benzodiazepine‐like properties and for hypnotic, neuroleptic and antidepressant properties, in order to complete the study of dose‐dependent sedative and analgesic effects previously demonstrated. The plant extract did not protect mice against the convulsant effects of pentylenetetrazol, it did not cause muscle relaxant effects and it did not seem to possess any affinity for benzodiazepine receptors. In addition, Eh did not have its own hypnotic effects in mice, but it intensified those of barbiturates, and caused a direct action on the central nervous system. This aqueous extract did not possess neuroleptic activity, but slight antidepressant effects were obtained against reserpine‐induced ptosis and oxotremorine‐induced hypothermia.
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