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Hcrtr1 and 2 signaling differentially regulates depression-like behaviors.

机译:Hcrtr1和2信号差异调节抑郁样行为。

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The orexin/hypocretin system has the potential to significantly modulate affect, based on both the neuroanatomical projection patterns of these neurons and on the sites of orexin receptor expression. However, there is little data supporting the role of specific orexin receptors in the modulation of depression-like behavior. Here we report behavioral profiling of mice after genetic or pharmacologic inhibition of hcrtr1 and 2 receptor signaling. Hcrtr1 null mice displayed a significant reduction in behavioral despair in the forced swim test and tail suspension test. Wild-type mice treated with the hcrtr1 antagonist SB-334867 also displayed a similar reduction in behavioral despair. No difference in anxiety-like behavior was noted following hcrtr1 deletion. In contrast, hcrtr2-null mice displayed an increase in behavioral despair with no effect on measures of anxiety. These studies suggest that the balance of orexin action at either the hcrtr1 or the hcrtr2 receptor produces an anti-depressant or pro-depressant like effect, depending on the receptor subtype activated.
机译:基于这些神经元的神经解剖学投影模式以及基于orexin受体表达的位点,orexin / hypocretin系统具有显着调节作用的潜力。然而,几乎没有数据支持特定的食欲素受体在抑郁样行为的调节中的作用。在这里,我们报告了hcrtr1和2受体信号传导的遗传或药理抑制后的小鼠行为分析。 Hcrtr1空小鼠在强迫游泳试验和尾巴悬吊试验中表现出极大的行为绝望减少。用hcrtr1拮抗剂SB-334867处理的野生型小鼠也表现出类似的行为绝望减少。 hcrtr1删除后,未注意到焦虑样行为的差异。相反,hcrtr2-null小鼠表现出行为绝望的增加,而对焦虑的测量没有影响。这些研究表明,食欲蛋白在hcrtr1或hcrtr2受体上的作用平衡会产生抗抑郁药或促抑郁药样作用,具体取决于激活的受体亚型。

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