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D [29], with ?purity greater than 98 . All other chemicals were of analytical grade and obtained from standard commercial suppliers. S-(+)Dicentrine was dissolved in 1 DMSO (Merck, Germany) and 5 Tween 80 (CRQ, Brazil) plus saline (NaCl 0.9 ), CFA, AMG9810 and cinnamaldehyde were dissolved in 1 Tween 80 plus saline, and all other drugs were dissolved in saline. The final concentration of Tween 80 or DMSO did not exceed 5 and 1 respectively and did not cause any effect per se.Statistical AnalysisResults are presented as mean 6 S.E.M. and the data were analyzed by one-way 10457188 analysis of variance (ANOVA) followed byFigure 1. Effect of S-(+)-dicentrine (DCTN, 100 mg/kg, p.o.) on mechanical hypersensitivity induced by CFA 50 . On 1st and 14th days, evaluations were done 1, 2, 3, 4 and 24 hours post-DCTN treatment; all other evaluations were done 1 hour post-treatment. Each point represents the mean 6 S.E.M. of 8 animals and significance levels are indicated by *p,0.05 and **p,0.01 when compared to the CFA i.pl. group (two-way anova and Bonferroni post hoc test). doi:10.1371/journal.pone.0067730.gS-(+)-Dicentrine Induces AntinociceptionFigure 2. Effect of S-(+)-dicentrine (DCTN, 100 mg/kg, p.o.) on mechanical hypersensitivity induced by CFA 80 . Panel A: time-course effect of DCTN evaluated at 1, 2, 3, 4 and 24 hours post-DCTN administration; each point represents the mean 6 S.E.M. of 10 animals and significance levels are indicated by *p,0.05 and ***p,0.001 when compared to the CFA i.pl. group (two-way anova and Bonferroni post hoc test). Panel B: effect of DCTN on 7th and 10th days post-CFA injection, evaluated before DCTN administration (basal) and 1 hour post-DCTN administration; each bar represents the mean 6 S.E.M. of 10 animals and significance levels are indicated by ***p,0.001 when compared to control group and ##p,0.01 when compared to the respective basal of CFA i.pl. group (one-way anova and Student-Newman-Keuls post hoc test). doi:10.1371/journal.pone.0067730.gCFA-induced Thermal HypersensitivityHypersensitivity to cold stimulus was evaluated at 2nd, 4th and 7th day post-CFA injection and as showed in Fig. 3A, S-(+)dicentrine (100 mg/kg, p.o.) was able to reduce the responses to acetone with inhibitions of 7966 , 8664 and 100 on 2nd, 4th, 7th days, respectively. S-(+)-Dicentrine had no effect per se (data not shown). However, when evaluated in the hot-plate, dicentrine did not increase the latency time for paw withdrawal, indicating no effect on heat hypersensitivity (Fig. 3B).Capsaicin and Cinnamaldehyde-induced NociceptionSince S-(+)-dicentrine reduced hypersensitivity to cold, but not to heat, we further investigated if the thermo-TRPs (TRPV1 and TRPA1 ion channels) would be involved in on its effect. As showed in Fig. 4, the TRPV1 activator capsaicin induced a lickingbehavior characteristic of nociception, which was reduced by the TRPV1 80-49-9 cost antagonist AMG9810, either when administered by intraperitoneal or intraplantar routes, but not by S-(+)-dicentrine. However, as showed in Fig. 5, S-(+)-dicentrine was able to reduce the licking time induced by cinnamaldehyde, a TRPA1 activator, either when administered by oral route (100 mg/kg) or intraplantar (100 mg/paw), with inhibitions of 7561 and 5368 , respectively, 34540-22-2 web similarly to the TRPA1 blocker camphor. Given the indicative participation of TRPA1 on S-(+)-dicentrine effect, a dose-response curve was made evaluating both spontaneous nociception and cold hypersensitivity. As demons.D [29], with ?purity greater than 98 . All other chemicals were of analytical grade and obtained from standard commercial suppliers. S-(+)Dicentrine was dissolved in 1 DMSO (Merck, Germany) and 5 Tween 80 (CRQ, Brazil) plus saline (NaCl 0.9 ), CFA, AMG9810 and cinnamaldehyde were dissolved in 1 Tween 80 plus saline, and all other drugs were dissolved in saline. The final concentration of Tween 80 or DMSO did not exceed 5 and 1 respectively and did not cause any effect per se.Statistical AnalysisResults are presented as mean 6 S.E.M. and the data were analyzed by one-way 10457188 analysis of variance (ANOVA) followed byFigure 1. Effect of S-(+)-dicentrine (DCTN, 100 mg/kg, p.o.) on mechanical hypersensitivity induced by CFA 50 . On 1st and 14th days, evaluations were done 1, 2, 3, 4 and 24 hours post-DCTN treatment; all other evaluations were done 1 hour post-treatment. Each point represents the mean 6 S.E.M. of 8 animals and significance levels are indicated by *p,0.05 and **p,0.01 when compared to the CFA i.pl. group (two-way anova and Bonferroni post hoc test). doi:10.1371/journal.pone.0067730.gS-(+)-Dicentrine Induces AntinociceptionFigure 2. Effect of S-(+)-dicentrine (DCTN, 100 mg/kg, p.o.) on mechanical hypersensitivity induced by CFA 80 . Panel A: time-course effect of DCTN evaluated at 1, 2, 3, 4 and 24 hours post-DCTN administration; each point represents the mean 6 S.E.M. of 10 animals and significance levels are indicated by *p,0.05 and ***p,0.001 when compared to the CFA i.pl. group (two-way anova and Bonferroni post hoc test). Panel B: effect of DCTN on 7th and 10th days post-CFA injection, evaluated before DCTN administration (basal) and 1 hour post-DCTN administration; each bar represents the mean 6 S.E.M. of 10 animals and significance levels are indicated by ***p,0.001 when compared to control group and ##p,0.01 when compared to the respective basal of CFA i.pl. group (one-way anova and Student-Newman-Keuls post hoc test). doi:10.1371/journal.pone.0067730.gCFA-induced Thermal HypersensitivityHypersensitivity to cold stimulus was evaluated at 2nd, 4th and 7th day post-CFA injection and as showed in Fig. 3A, S-(+)dicentrine (100 mg/kg, p.o.) was able to reduce the responses to acetone with inhibitions of 7966 , 8664 and 100 on 2nd, 4th, 7th days, respectively. S-(+)-Dicentrine had no effect per se (data not shown). However, when evaluated in the hot-plate, dicentrine did not increase the latency time for paw withdrawal, indicating no effect on heat hypersensitivity (Fig. 3B).Capsaicin and Cinnamaldehyde-induced NociceptionSince S-(+)-dicentrine reduced hypersensitivity to cold, but not to heat, we further investigated if the thermo-TRPs (TRPV1 and TRPA1 ion channels) would be involved in on its effect. As showed in Fig. 4, the TRPV1 activator capsaicin induced a lickingbehavior characteristic of nociception, which was reduced by the TRPV1 antagonist AMG9810, either when administered by intraperitoneal or intraplantar routes, but not by S-(+)-dicentrine. However, as showed in Fig. 5, S-(+)-dicentrine was able to reduce the licking time induced by cinnamaldehyde, a TRPA1 activator, either when administered by oral route (100 mg/kg) or intraplantar (100 mg/paw), with inhibitions of 7561 and 5368 , respectively, similarly to the TRPA1 blocker camphor. Given the indicative participation of TRPA1 on S-(+)-dicentrine effect, a dose-response curve was made evaluating both spontaneous nociception and cold hypersensitivity. As demons.

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Author: calcimimeticagent