目的研究侧脑室注射不同剂量orexin2A对麻醉大鼠脑电图(electroencephalogram,EEG)、翻正反射消失(loss of righting reflex,LRR)持续时间、共济失调等的影响。方法腹腔注射氯胺酮75mg/kg及咪达唑仑5mg/kg麻醉大鼠后,侧脑室注射不同剂量...目的研究侧脑室注射不同剂量orexin2A对麻醉大鼠脑电图(electroencephalogram,EEG)、翻正反射消失(loss of righting reflex,LRR)持续时间、共济失调等的影响。方法腹腔注射氯胺酮75mg/kg及咪达唑仑5mg/kg麻醉大鼠后,侧脑室注射不同剂量orexin2A,通过大鼠脑电δ波比例、LRR持续时间及共济失调监测,了解不同剂量orexin2A对麻醉大鼠催醒效果。结果与对照组相比,侧脑室注射orexin2A1nmol后,大鼠脑电δ波、LRR持续时间及共济失调时间,差异无统计学意义(P>0.05);侧脑室注射orexin2A4、7、10nmol后,大鼠脑电δ波、LRR持续时间及共济失调时间,差异有统计学意义(t=22.81~36.45,P<0.01);高剂量组与超高剂量组比较,差异无统计学意义(P>0.05)。结论侧脑室注射orexin2A可使麻醉深度变浅,麻醉时间缩短,并可促进麻醉后运动功能恢复,存在一定的量效关系。展开更多
Orexin signaling has been associated with energy expenditure and brown adipose tissue(BAT)function.However,conflicting data exist in the field about how orexin signaling regulates BAT thermogenesis.In this study,we sh...Orexin signaling has been associated with energy expenditure and brown adipose tissue(BAT)function.However,conflicting data exist in the field about how orexin signaling regulates BAT thermogenesis.In this study,we show that a specific orexin receptor type 2(OX2R)agonist[Ala11,D-Leu15]-OxB(OB-Ala)inhibited intrascapular brown adipose tissue(iBAT)thermogenesis by reducing sympathetic output to iBAT.This effect is mediated by OX2Rs located on afferent nerve endings innervating iBAT instead of brown adipocyte itself.Microinjection of OB-Ala into iBAT inhibited iBAT thermogenesis in mice upon cold exposure and neuronal activity in the paraventricular nucleus.Findings suggest that OB-Ala could inhibit iBAT thermogenesis by attenuating sensory input thereby inhibiting the sympathetic-sensory iBAT feedback loop.Our study uncovers a novel primary action site of orexin in the regulation of energy balance.展开更多
文摘目的研究侧脑室注射不同剂量orexin2A对麻醉大鼠脑电图(electroencephalogram,EEG)、翻正反射消失(loss of righting reflex,LRR)持续时间、共济失调等的影响。方法腹腔注射氯胺酮75mg/kg及咪达唑仑5mg/kg麻醉大鼠后,侧脑室注射不同剂量orexin2A,通过大鼠脑电δ波比例、LRR持续时间及共济失调监测,了解不同剂量orexin2A对麻醉大鼠催醒效果。结果与对照组相比,侧脑室注射orexin2A1nmol后,大鼠脑电δ波、LRR持续时间及共济失调时间,差异无统计学意义(P>0.05);侧脑室注射orexin2A4、7、10nmol后,大鼠脑电δ波、LRR持续时间及共济失调时间,差异有统计学意义(t=22.81~36.45,P<0.01);高剂量组与超高剂量组比较,差异无统计学意义(P>0.05)。结论侧脑室注射orexin2A可使麻醉深度变浅,麻醉时间缩短,并可促进麻醉后运动功能恢复,存在一定的量效关系。
基金supported by grants from the National Natural Science Foundation of China (Grants No. 31800971 and 81873654)
文摘Orexin signaling has been associated with energy expenditure and brown adipose tissue(BAT)function.However,conflicting data exist in the field about how orexin signaling regulates BAT thermogenesis.In this study,we show that a specific orexin receptor type 2(OX2R)agonist[Ala11,D-Leu15]-OxB(OB-Ala)inhibited intrascapular brown adipose tissue(iBAT)thermogenesis by reducing sympathetic output to iBAT.This effect is mediated by OX2Rs located on afferent nerve endings innervating iBAT instead of brown adipocyte itself.Microinjection of OB-Ala into iBAT inhibited iBAT thermogenesis in mice upon cold exposure and neuronal activity in the paraventricular nucleus.Findings suggest that OB-Ala could inhibit iBAT thermogenesis by attenuating sensory input thereby inhibiting the sympathetic-sensory iBAT feedback loop.Our study uncovers a novel primary action site of orexin in the regulation of energy balance.
