The aim of this work was evaluate the effects of terpinolene on acute inflammatory responses in mice.In vivo preclinical research using different inflammatory agents to induce acute responses and evaluate the effects ...The aim of this work was evaluate the effects of terpinolene on acute inflammatory responses in mice.In vivo preclinical research using different inflammatory agents to induce acute responses and evaluate the effects of terpinolene in orally treated mice.The acute inflammatory responses were induced by injecting phlogistic agents in the mice paw to observe the development of pain responses(formalin test)or edema(carrageenan,dextran,histamine,arachidonic acid,and prostaglandin).The antiedematogenic activity was also evaluated using a croton oil-induced ear edema model.Finally,cotton pellet-induced granuloma was used to carry out a pre-liminary evaluation of terpinolene in a chronic inflammatory model.Topically administered terpinolene(5,10,and 20 mg/mL)significantly inhibited ear edema development(by 33.82%,29.63%,and 33,30%,respectively).Following an oral administration,only the highest dose of the monoterpene(200 mg/kg)reduced the licking time of the formalin test in both phases 1(73.55%)and 2(96.61%).The carrageenan-induced edema signifi-cantly inhibited over time following the oral administration of terpinolene at 50 mg/kg(T1:47.74%,T2:54.67%,T3:48.63%,and T4:62.99%),100 mg/kg(T1:72.86%,T2:71.03%,T3:48.63%,and T4:57.83%),and 200 mg/kg(T1:43.22%,T2:34.11%,T3:36.47%,and T4:45.20%).On the other hand,only the dose of 200 (mg/kg)caused a significant reduction of the dextran-induced paw edema(T1:51.18%,T2:60%,T3:50.92%,and T4:65.15%).Regarding the participation of inflammatory pathways,the monoterpene(200 mg/kg,p.o.)had little impact on histamine-induced edema,while the edema induced by arachidonic acid was significantly reduced at all time-points(T1:37.04%,T2:24.32%,and T3:35.13%,and T4:35.53%),which was corroborated by the observation that the compound inhibited the response triggered by prostaglandin E2(PGE2),suggesting inter-ference with downstream signaling cascades.Finally,terpinolene(200 mg/kg,p.o.)reduced both the weight(21.43%)and total protein content(36.21%)of the cotton pellet-induced granuloma,indicating an anti-inflammatory activity in this chronic model.Terpinolene inhibited acute inflammatory responses and reduced granuloma development in vivo,possibly by interfering with the tissue changes orchestrated by inflammatory mediators such as histamine and PGE2.However,the molecular mechanisms underlying this pharmacological observation need to be confirmed by further research.展开更多
The title compound,(1S,4R)-4,7,7-trimethyl-6-oxabicyclo [3.2.1] octane-1,4-diol(C(10)H(18)O3), has been synthesized from terpinolene via one-step catalytic synthetic method and structurally characterized by me...The title compound,(1S,4R)-4,7,7-trimethyl-6-oxabicyclo [3.2.1] octane-1,4-diol(C(10)H(18)O3), has been synthesized from terpinolene via one-step catalytic synthetic method and structurally characterized by means of HRMS, IR, 1H-NMR, (13)C-NMR and single-crystal X-ray diffraction. The compound crystallizes in trigonal, space group R-3, with a = 27.892(9), b = 27.892(9), c = 6.720(2) A, γ = 120°, Z = 18, V = 4527(3) A3, Dc = 1.230 g/cm3, Mr = 186.24, λ(Mo Kα) = 0.71073?, μ = 0.09 mm(-1), F(000) = 1836, the final R = 0.051 and wR = 0.161. The title compound molecule contained a 6-oxabicyclo[3.2.1]octane skeleton and two hydroxyl groups, which were connected through intermolecular O–H…O hydrogen bonds to generate a two-dimensional network. Especially, the preliminary bioassay showed that the title compound can promote the root growth and shoot elongation of rape(Brassica campestris) at low concentration(0.62570 mmol·L^-1) and inhibit them at high concentration(〉 70 mmol·L^-1).展开更多
基金financial support provided of support of the Brazilian agencies CAPES,FUNCAP,CNPq,and FINEPNacional Institute of Science and Technology-Ethnobiology,Bioprospecting and Nature Conservation/CNPq/FACEPE.
文摘The aim of this work was evaluate the effects of terpinolene on acute inflammatory responses in mice.In vivo preclinical research using different inflammatory agents to induce acute responses and evaluate the effects of terpinolene in orally treated mice.The acute inflammatory responses were induced by injecting phlogistic agents in the mice paw to observe the development of pain responses(formalin test)or edema(carrageenan,dextran,histamine,arachidonic acid,and prostaglandin).The antiedematogenic activity was also evaluated using a croton oil-induced ear edema model.Finally,cotton pellet-induced granuloma was used to carry out a pre-liminary evaluation of terpinolene in a chronic inflammatory model.Topically administered terpinolene(5,10,and 20 mg/mL)significantly inhibited ear edema development(by 33.82%,29.63%,and 33,30%,respectively).Following an oral administration,only the highest dose of the monoterpene(200 mg/kg)reduced the licking time of the formalin test in both phases 1(73.55%)and 2(96.61%).The carrageenan-induced edema signifi-cantly inhibited over time following the oral administration of terpinolene at 50 mg/kg(T1:47.74%,T2:54.67%,T3:48.63%,and T4:62.99%),100 mg/kg(T1:72.86%,T2:71.03%,T3:48.63%,and T4:57.83%),and 200 mg/kg(T1:43.22%,T2:34.11%,T3:36.47%,and T4:45.20%).On the other hand,only the dose of 200 (mg/kg)caused a significant reduction of the dextran-induced paw edema(T1:51.18%,T2:60%,T3:50.92%,and T4:65.15%).Regarding the participation of inflammatory pathways,the monoterpene(200 mg/kg,p.o.)had little impact on histamine-induced edema,while the edema induced by arachidonic acid was significantly reduced at all time-points(T1:37.04%,T2:24.32%,and T3:35.13%,and T4:35.53%),which was corroborated by the observation that the compound inhibited the response triggered by prostaglandin E2(PGE2),suggesting inter-ference with downstream signaling cascades.Finally,terpinolene(200 mg/kg,p.o.)reduced both the weight(21.43%)and total protein content(36.21%)of the cotton pellet-induced granuloma,indicating an anti-inflammatory activity in this chronic model.Terpinolene inhibited acute inflammatory responses and reduced granuloma development in vivo,possibly by interfering with the tissue changes orchestrated by inflammatory mediators such as histamine and PGE2.However,the molecular mechanisms underlying this pharmacological observation need to be confirmed by further research.
基金Supported by the National Natural Science Foundation of China(No.31460174)the Science and Research Start-Up Project for the Recruit Talent of Guangxi University for Nationalities(No.2014MDQD014)Innovation Project of Guangxi Graduate Education(gxun-chxzs2016113)
文摘The title compound,(1S,4R)-4,7,7-trimethyl-6-oxabicyclo [3.2.1] octane-1,4-diol(C(10)H(18)O3), has been synthesized from terpinolene via one-step catalytic synthetic method and structurally characterized by means of HRMS, IR, 1H-NMR, (13)C-NMR and single-crystal X-ray diffraction. The compound crystallizes in trigonal, space group R-3, with a = 27.892(9), b = 27.892(9), c = 6.720(2) A, γ = 120°, Z = 18, V = 4527(3) A3, Dc = 1.230 g/cm3, Mr = 186.24, λ(Mo Kα) = 0.71073?, μ = 0.09 mm(-1), F(000) = 1836, the final R = 0.051 and wR = 0.161. The title compound molecule contained a 6-oxabicyclo[3.2.1]octane skeleton and two hydroxyl groups, which were connected through intermolecular O–H…O hydrogen bonds to generate a two-dimensional network. Especially, the preliminary bioassay showed that the title compound can promote the root growth and shoot elongation of rape(Brassica campestris) at low concentration(0.62570 mmol·L^-1) and inhibit them at high concentration(〉 70 mmol·L^-1).
