Autor(es): Lima, Milena da Silva ; Evangelista, Afrânio Ferreira ; Santos, Gisele Graça Leite dos ; Ribeiro, Ivone Maria ; Tomassini, Therezinha Coelho Barbosa ; Soares, Milena Botelho Pereira ; Villarreal, Cristiane Flora
Data: 2015
Origem: Oasisbr
Autor(es): Lima, Milena da Silva ; Evangelista, Afrânio Ferreira ; Santos, Gisele Graça Leite dos ; Ribeiro, Ivone Maria ; Tomassini, Therezinha Coelho Barbosa ; Soares, Milena Botelho Pereira ; Villarreal, Cristiane Flora
Data: 2015
Origem: Oasisbr
Texto completo: acesso restrito. p.2397−2403
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Pain is the most common reason a patient sees a physician. Nevertheless, the use of typical painkillers is not completely effective in controlling all pain syndromes; therefore further attempts have been made to develop improved analgesic drugs. The present study was undertaken to evaluate the antinociceptive properties of physalins B (1), D (2), F (3), and G (4) isolated from Physalis angulata in inflammatory and centrally mediated pain tests in mice. Systemic pretreatment with 1–4 produced dose-related antinociceptive effects on the writhing and formalin tests, traditional screening tools for the assessment of analgesic drugs. On the other hand, only 3 inhibited inflammatory parameters such as hyperalgesia, edema, and local production of TNF-α following induction with complete Freund’s adjuvant. Treatment with 1, 3, and 4 produced an antinociceptive effect on the tail flick test, suggesting a centrally mediated antinociception. Reinforcing this idea, 2–4 enhanced the mice latency reaction time during the hot plate test. Mice treated with physalins did not demonstrate motor performance alterations. These results suggest that 1–4 present antinociceptive properties associated with central, but not anti-inflammatory, events and indicate a new pharmacological property of physalins.