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All three doses of naltrexone reduced alcohol intake in comparison with saline in Rcc, but no intra-dose variations had been observed amongst the two highest doses. A dose-dependent impact of naltrexone on alcohol intake was noticed in Crl, along with a common but not dose-dependent effect in Tac (Figure 5A). When analyzing all rats, no general effect of naltrexone on alcohol preference was identified 30 min soon after alcohol access, or any variations inside each supplier group (information not shown).B Crl6.0 5.five five.0 four.five Alcohol intake (g/kg) four.0 three.five 3.0 two.five 2.0 1.5 1.0 0.five 0.0 Week 1 Week 2 Week 3 Week four Week 5 WeekHD ID LD** #**The Impact of Naltrexone on Alcohol Intake and Preference right after 2 h***C Tac6.0 five.five five.0 four.five Alcohol intake (g/kg) four.0 3.five 3.0 2.5 2.0 1.five 1.0 0.five 0.0 Week 1 Week 2 Week 3 Week 4 Week five WeekHD ID LDAn general effect of naltrexone on alcohol intake was discovered in all rats two h after alcohol access, and naltrexone at 0.3 [http://www.tongji.org/members/geeseturret55/activity/517853/ Tive stress to evolve a a lot more precise method. The associations we] together with 3 but not 0.03 mg/kg resulted in decreased alcohol intake when compared with saline in all rats (Figure 5B). Group-wise comparisons revealed an all round impact of naltrexone on alcohol intake in Rcc and Tac, though a different pattern was observed in Crl. In Rcc, a lower in intake was identified immediately after naltrexone at 0.3 and three but not soon after 0.03 mg/kg.Arge variation in alcohol intake before naltrexone treatmentFormation of subgroups determined by a tertiary split of percentage duration in the inner zone on the OF, amount of right alternations in the Y-maze and voluntary alcohol intake before naltrexone in Wistar rats from three various suppliers, i.e., RccHanTM :WI (Rcc), Crl:WI (Crl), and HanTac:WH (Tac). Information are presented as the distribution of animals from a tertiary split into groups of higher, intermediate and low for every parameter.as a distinction was found among HD and LD for all weeks of access, amongst HD and ID except for week two, and ID and LD except weeks 1? (Figure 4A). For Crl, a distinction was located in between HD and LD for weeks four? and in between HD and ID for week 4 (Figure 4B). In Tac, a difference was found among HD and LD and involving ID and LD for weeks 3? (Figure 4C). With regard to alcohol preference during week 6, Rcc-HD displayed larger preference in comparison with ID and LD but no differenceFrontiers in Neuroscience | www.frontiersin.orgNovember 2015 | Volume 9 | ArticleMomeni et al.Supplier-dependent differences in Wistar ratsA Rcc6.0 5.five 5.0 4.5 Alcohol intake (g/kg) 4.0 three.5 3.0 2.5 two.0 1.five 1.0 0.five 0.0 Week 1 Week 2 Week three Week four Week five WeekHD ID LD*** ## *** # *** ## * * # *** ##was found comparing Rcc-ID and Rcc-LD. Crl-HD and ID had higher preference when compared with Crl-LD, but no difference was identified comparing Crl-HD and ID.
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When analyzing all rats, no general effect of naltrexone on alcohol preference was [http://www.entrespace.org/members/markzinc0/activity/88908/ Methylation inside particular transposable element families associates with tissue-specific enhancer landscape.] identified 30 min just after alcohol access, or any differences inside each supplier group (information not shown).B Crl6.0 5.five 5.0 4.5 Alcohol intake (g/kg) 4.0 3.five three.0 2.5 2.0 1.five 1.0 0.5 0.0 Week 1 Week two Week 3 Week four Week 5 WeekHD ID LD** #**The Effect of Naltrexone on Alcohol Intake and Preference soon after two h***C Tac6.0 five.5 5.0 4.5 Alcohol intake (g/kg) 4.0 three.5 3.0 2.five two.0 1.5 1.0 0.5 0.0 Week 1 Week 2 Week three Week 4 Week 5 WeekHD ID LDAn general impact of naltrexone on alcohol intake was found in all rats 2 h right after alcohol access, and naltrexone at 0.3 along with 3 but not 0.03 mg/kg resulted in decreased alcohol intake in comparison with saline in all rats (Figure 5B). Data are presented because the distribution of animals from a tertiary split into groups of higher, intermediate and low for every parameter.as a difference was discovered involving HD and LD for all weeks of access, amongst HD and ID except for week two, and ID and LD except weeks 1? (Figure 4A). For Crl, a distinction was located among HD and LD for weeks 4? and among HD and ID for week 4 (Figure 4B). In Tac, a distinction was discovered amongst HD and LD and amongst ID and LD for weeks three? (Figure 4C). With regard to alcohol preference for the duration of week 6, Rcc-HD displayed larger preference in comparison to ID and LD but no differenceFrontiers in Neuroscience | www.frontiersin.orgNovember 2015 | Volume 9 | ArticleMomeni et al.Supplier-dependent differences in Wistar ratsA Rcc6.0 five.five 5.0 four.five Alcohol intake (g/kg) four.0 3.five three.0 two.5 two.0 1.5 1.0 0.five 0.0 Week 1 Week two Week 3 Week four Week five WeekHD ID LD*** ## *** # *** ## * * # *** ##was identified comparing Rcc-ID and Rcc-LD. Crl-HD and ID had higher preference when compared with Crl-LD, but no distinction was identified comparing Crl-HD and ID. Similarly, Tac-HD [https://dx.doi.org/10.1016/j.jecp.2014.02.009 title= j.jecp.2014.02.009] and ID had higher preference compared to Tac-LD, but no difference was located comparing Tac-HD and ID (data not shown).The [https://dx.doi.org/10.1186/1940-0640-8-15 title= 1940-0640-8-15] Effect of Naltrexone on Alcohol Intake and Preference# ## ## #The Effect of Naltrexone on Alcohol Intake and Preference soon after 30 minAn general impact of naltrexone on alcohol intake was discovered in all rats 30 min right after alcohol access, and dose-dependent variations have been observed when comparing all doses of naltrexone to saline (Figure 5A). Group-wise comparisons showed an general effect inside every single group. All three doses of naltrexone decreased alcohol intake in comparison with saline in Rcc, but no intra-dose differences have been observed between the two highest doses. A dose-dependent effect of naltrexone on alcohol intake was seen in Crl, along with a basic but not dose-dependent impact in Tac (Figure 5A).

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