Antinociceptive effect of geranylgeraniol and 6α,7β-dihydroxyvouacapan-17β-oate methyl ester isolated from Pterodon pubescens Benth
Abstract Background Pterodon pubescens Benth seeds are commercially available in the Brazilian medicinal plant street market. The crude alcoholic extracts of this plant are used in folk medicine as anti-inflammatory, analgesic, and anti-rheumatic preparations. The aim of this study was to evaluate t...
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| Published in | BMC pharmacology Vol. 10; no. 1; p. 1 |
|---|---|
| Main Authors | , , , , , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
BioMed Central Ltd
07.01.2010
BioMed Central |
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| Abstract | Abstract
Background
Pterodon pubescens
Benth seeds are commercially available in the Brazilian medicinal plant street market. The crude alcoholic extracts of this plant are used in folk medicine as anti-inflammatory, analgesic, and anti-rheumatic preparations. The aim of this study was to evaluate the contribution of geranylgeraniol (C1) and 6α, 7β-dihydroxyvouacapan-17β-oate methyl ester (C2) isolated from
Pterodon pubescens
Benth. to the antinociceptive activity of the crude extract.
Results
Compounds C1 and C2 demonstrated activity against writhing with intraperitoneal (i.p.) and oral (p.o.) routes, capsaicin (i.p. and p.o.), glutamate (i.p.), and in the hot-plate (p.o.) tests, demonstrating their contribution to the antinociceptive activity of crude
Pterodon pubescens
Benth extracts. The observed activity of compounds C1 and C2 may be related to vanilloid receptors VR1, and/or glutamate peripheral receptors. In hot-plate model, the antinociceptive activity was maintained when naloxone chloride (opioid antagonist) was administered prior to treatment with compounds suggesting that C1 and C2 (p.o.) do not exert their antinociceptive effects in the hot-plate test via opioid receptors. The findings presented herein also suggest that compounds within the crude
Pterodon pubescens
Benth. extract may exert a synergistic interactive effect, since the crude extract (300 mg.kg
-1
) containing lower concentrations of compounds C1 (11.5%- 34.6 mg. kg
-1
) and C2 (1.5% - 4.7 mg.kg
-1
) gave statistically the same effect to the pure compounds when tested separately (C1 = C2 = 300 mg.kg
-1
) in writhing experimental model with p.o. administration. Further studies will be undertaken to establish more specifically the mechanisms of action for compounds C1 and C2. Possible synergistic interactions will be evaluated employing the Isobole method.
Conclusion
These results allowed us to establish a relationship between the popular use of
Pterodon pubescens
seeds for pain relief and the activity of two major compounds isolated from this species which demonstrated antinociceptive activity. Various "
in vivo"
experimental models corroborate the folk use of this species for different pain and inflammation disorders. |
|---|---|
| AbstractList | Abstract
Background
Pterodon pubescens
Benth seeds are commercially available in the Brazilian medicinal plant street market. The crude alcoholic extracts of this plant are used in folk medicine as anti-inflammatory, analgesic, and anti-rheumatic preparations. The aim of this study was to evaluate the contribution of geranylgeraniol (C1) and 6α, 7β-dihydroxyvouacapan-17β-oate methyl ester (C2) isolated from
Pterodon pubescens
Benth. to the antinociceptive activity of the crude extract.
Results
Compounds C1 and C2 demonstrated activity against writhing with intraperitoneal (i.p.) and oral (p.o.) routes, capsaicin (i.p. and p.o.), glutamate (i.p.), and in the hot-plate (p.o.) tests, demonstrating their contribution to the antinociceptive activity of crude
Pterodon pubescens
Benth extracts. The observed activity of compounds C1 and C2 may be related to vanilloid receptors VR1, and/or glutamate peripheral receptors. In hot-plate model, the antinociceptive activity was maintained when naloxone chloride (opioid antagonist) was administered prior to treatment with compounds suggesting that C1 and C2 (p.o.) do not exert their antinociceptive effects in the hot-plate test via opioid receptors. The findings presented herein also suggest that compounds within the crude
Pterodon pubescens
Benth. extract may exert a synergistic interactive effect, since the crude extract (300 mg.kg
-1
) containing lower concentrations of compounds C1 (11.5%- 34.6 mg. kg
-1
) and C2 (1.5% - 4.7 mg.kg
-1
) gave statistically the same effect to the pure compounds when tested separately (C1 = C2 = 300 mg.kg
-1
) in writhing experimental model with p.o. administration. Further studies will be undertaken to establish more specifically the mechanisms of action for compounds C1 and C2. Possible synergistic interactions will be evaluated employing the Isobole method.
Conclusion
These results allowed us to establish a relationship between the popular use of
Pterodon pubescens
seeds for pain relief and the activity of two major compounds isolated from this species which demonstrated antinociceptive activity. Various "
in vivo"
experimental models corroborate the folk use of this species for different pain and inflammation disorders. BACKGROUND: Pterodon pubescens Benth seeds are commercially available in the Brazilian medicinal plant street market. The crude alcoholic extracts of this plant are used in folk medicine as anti-inflammatory, analgesic, and anti-rheumatic preparations. The aim of this study was to evaluate the contribution of geranylgeraniol (C1) and 6α, 7β-dihydroxyvouacapan-17β-oate methyl ester (C2) isolated from Pterodon pubescens Benth. to the antinociceptive activity of the crude extract. RESULTS: Compounds C1 and C2 demonstrated activity against writhing with intraperitoneal (i.p.) and oral (p.o.) routes, capsaicin (i.p. and p.o.), glutamate (i.p.), and in the hot-plate (p.o.) tests, demonstrating their contribution to the antinociceptive activity of crude Pterodon pubescens Benth extracts. The observed activity of compounds C1 and C2 may be related to vanilloid receptors VR1, and/or glutamate peripheral receptors. In hot-plate model, the antinociceptive activity was maintained when naloxone chloride (opioid antagonist) was administered prior to treatment with compounds suggesting that C1 and C2 (p.o.) do not exert their antinociceptive effects in the hot-plate test via opioid receptors. The findings presented herein also suggest that compounds within the crude Pterodon pubescens Benth. extract may exert a synergistic interactive effect, since the crude extract (300 mg.kg-1) containing lower concentrations of compounds C1 (11.5%- 34.6 mg. kg-1) and C2 (1.5% - 4.7 mg.kg-1) gave statistically the same effect to the pure compounds when tested separately (C1 = C2 = 300 mg.kg-1) in writhing experimental model with p.o. administration. Further studies will be undertaken to establish more specifically the mechanisms of action for compounds C1 and C2. Possible synergistic interactions will be evaluated employing the Isobole method. CONCLUSION: These results allowed us to establish a relationship between the popular use of Pterodon pubescens seeds for pain relief and the activity of two major compounds isolated from this species which demonstrated antinociceptive activity. Various "in vivo" experimental models corroborate the folk use of this species for different pain and inflammation disorders. |
| ArticleNumber | 1 |
| Author | Eberlin, Marcos N Carvalho, João E Cabral, Elaine Foglio, Mary A Rodrigues, Rodney AF Tamashiro, Jorge Y Sousa, Ilza MO Spindola, Humberto M Servat, Leila Denny, Carina |
| AuthorAffiliation | 3 Biology Institute, State University of Campinas, P.O. Box 6109, 13083-970 Campinas-SP, Brazil 2 Department of Pharmacology, Anesthesiology and Therapeutics, Faculty of Dentistry, State University of Campinas, P.O. Box 52, 13414-903 Piracicaba-SP, Brazil 5 Chemistry Institute - São Paulo University, P. O. Box 26.077, 05513-970 São Paulo - SP, Brazil 1 CPQBA- State University of Campinas, P.O. Box 6171, 13083-970 Campinas-SP, Brazil 4 Thomson Mass Spectrometry Laboratory, Chemical Institute, State University of Campinas, P.O.BOX 6154, 13084-862 Campinas-SP, Brazil |
| AuthorAffiliation_xml | – name: 5 Chemistry Institute - São Paulo University, P. O. Box 26.077, 05513-970 São Paulo - SP, Brazil – name: 2 Department of Pharmacology, Anesthesiology and Therapeutics, Faculty of Dentistry, State University of Campinas, P.O. Box 52, 13414-903 Piracicaba-SP, Brazil – name: 4 Thomson Mass Spectrometry Laboratory, Chemical Institute, State University of Campinas, P.O.BOX 6154, 13084-862 Campinas-SP, Brazil – name: 1 CPQBA- State University of Campinas, P.O. Box 6171, 13083-970 Campinas-SP, Brazil – name: 3 Biology Institute, State University of Campinas, P.O. Box 6109, 13083-970 Campinas-SP, Brazil |
| Author_xml | – sequence: 1 givenname: Humberto M surname: Spindola fullname: Spindola, Humberto M – sequence: 2 givenname: Leila surname: Servat fullname: Servat, Leila – sequence: 3 givenname: Carina surname: Denny fullname: Denny, Carina – sequence: 4 givenname: Rodney AF surname: Rodrigues fullname: Rodrigues, Rodney AF – sequence: 5 givenname: Marcos N surname: Eberlin fullname: Eberlin, Marcos N – sequence: 6 givenname: Elaine surname: Cabral fullname: Cabral, Elaine – sequence: 7 givenname: Ilza MO surname: Sousa fullname: Sousa, Ilza MO – sequence: 8 givenname: Jorge Y surname: Tamashiro fullname: Tamashiro, Jorge Y – sequence: 9 givenname: João E surname: Carvalho fullname: Carvalho, João E – sequence: 10 givenname: Mary A surname: Foglio fullname: Foglio, Mary A |
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Background
Pterodon pubescens
Benth seeds are commercially available in the Brazilian medicinal plant street market. The crude alcoholic extracts of... BACKGROUND: Pterodon pubescens Benth seeds are commercially available in the Brazilian medicinal plant street market. The crude alcoholic extracts of this... |
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| Title | Antinociceptive effect of geranylgeraniol and 6α,7β-dihydroxyvouacapan-17β-oate methyl ester isolated from Pterodon pubescens Benth |
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