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雷美替胺和三唑仑在小鼠清晨觉醒基因模型中的作用。

Effects of ramelteon and triazolam in a mouse genetic model of early morning awakenings.

作者信息

Wisor Jonathan P, Jiang Peng, Striz Martin, O'Hara Bruce F

机构信息

Center for Neuroscience, SRI International, Menlo Park, CA 94025, USA.

出版信息

Brain Res. 2009 Nov 3;1296:46-55. doi: 10.1016/j.brainres.2009.07.103. Epub 2009 Aug 4.

Abstract

The onset of the daily wheel running bout precedes dark onset by several hours in the early runner genetic variant of mice. Here, we test the hypothesis that timed daily administration of a melatonin agonist, ramelteon, or a benzodiazepine, triazolam, normalizes the timing of daily wheel-running rhythms in early runner mice. The daily profiles of wheel-running activity of early runner mice were monitored continuously in a 12:12 light/dark cycle. Wheel running was assessed before, during and after timed daily oral administration of saline vehicle (n=12), ramelteon (10 mg/kg, n=12), or triazolam (1 mg/kg, n=12). The timing of wheel-running rhythms relative to the light/dark cycle was used as a measure of the timing of wake onset. Under baseline conditions, early runner mice entrained to a light/dark cycle at an advanced phase, approximately 3 h before dark onset, on average. Triazolam, but not ramelteon, suppressed wheel-running acutely when administered just prior to the time at which wheel-running onset had occurred under baseline conditions. On a washout day under a light/dark cycle subsequent to one week of once daily administration, the onset of wheel-running was delayed relative to baseline in both ramelteon-treated mice and triazolam-treated mice. In constant dark subsequent to a second week of once daily administration, the onset of wheel-running activity was not affected by either compound. Thus, ramelteon and triazolam caused a shift in the timing of wheel-running rhythms in an LD cycle but did so without long-term effects on the functioning of the circadian clock.

摘要

在小鼠的早期跑步者基因变体中,每日滚轮运动发作比黑暗开始提前数小时。在此,我们测试以下假设:每日定时给予褪黑素激动剂雷美替胺或苯二氮䓬类药物三唑仑,可使早期跑步者小鼠的每日滚轮运动节律时间正常化。在12:12光/暗循环中持续监测早期跑步者小鼠的滚轮运动活动的每日概况。在每日定时口服生理盐水载体(n = 12)、雷美替胺(10 mg/kg,n = 12)或三唑仑(1 mg/kg,n = 12)之前、期间和之后评估滚轮运动。相对于光/暗循环的滚轮运动节律时间用作觉醒开始时间的度量。在基线条件下,早期跑步者小鼠平均在黑暗开始前约3小时的提前阶段与光/暗循环同步。当在基线条件下滚轮运动开始时间之前给药时,三唑仑而非雷美替胺可急性抑制滚轮运动。在每日一次给药一周后的光/暗循环下的洗脱日,雷美替胺治疗组小鼠和三唑仑治疗组小鼠的滚轮运动开始相对于基线均延迟。在每日一次给药第二周后的持续黑暗中,滚轮运动活动的开始不受任何一种化合物的影响。因此,雷美替胺和三唑仑在LD循环中引起了滚轮运动节律时间的改变,但对生物钟功能没有长期影响。

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