Gladstone Institute of Neurological Disease, University of California, San Francisco, San Francisco, California 94158, USA.
J Neurosci. 2010 Feb 10;30(6):2160-4. doi: 10.1523/JNEUROSCI.5844-09.2010.
Adenosine A(2A) receptor antagonists are psychomotor stimulants that also hold therapeutic promise for movement disorders. However, the molecular mechanisms underlying their stimulant properties are not well understood. Here, we show that the robust increase in locomotor activity induced by an A(2A) antagonist in vivo is greatly attenuated by antagonizing cannabinoid CB(1) receptor signaling or by administration to CB(1)(-/-) mice. To determine the locus of increased endocannabinoid signaling, we measured the amount of anandamide [AEA (N-arachidonoylethanolamine)] and 2-arachidonoylglycerol (2-AG) in brain tissue from striatum and cortex. We find that 2-AG is selectively increased in striatum after acute blockade of A(2A) receptors, which are highly expressed by striatal indirect-pathway medium spiny neurons (MSNs). Using targeted whole-cell recordings from direct- and indirect-pathway MSNs, we demonstrate that A(2A) receptor antagonists potentiate 2-AG release and induction of long-term depression at indirect-pathway MSNs, but not direct-pathway MSNs. Together, these data outline a molecular mechanism by which A(2A) antagonists reduce excitatory synaptic drive on the indirect pathway through CB(1) receptor signaling, thus leading to increased psychomotor activation.
腺苷 A(2A)受体拮抗剂是一种精神运动兴奋剂,它们在运动障碍的治疗中也有很大的应用前景。然而,其兴奋剂特性的分子机制尚不清楚。在这里,我们发现体内 A(2A)拮抗剂引起的运动活性的显著增加,通过拮抗大麻素 CB(1)受体信号或在 CB(1)(-/-)小鼠中给药可以大大减弱。为了确定内源性大麻素信号增强的位置,我们测量了纹状体和皮质脑组织中花生四烯酸乙醇胺(AEA[N-花生四烯酰乙醇胺])和 2-花生四烯酰甘油(2-AG)的含量。我们发现,急性阻断 A(2A)受体后,2-AG 选择性地在纹状体中增加,而 A(2A)受体在纹状体间接途径中的中等棘突神经元(MSNs)中高度表达。使用直接和间接途径 MSNs 的靶向全细胞记录,我们证明 A(2A)受体拮抗剂增强了间接途径 MSNs 中的 2-AG 释放和长时程抑制的诱导,但不能增强直接途径 MSNs 中的 2-AG 释放和长时程抑制的诱导。综上所述,这些数据概述了 A(2A)拮抗剂通过 CB(1)受体信号减少间接途径上兴奋性突触传入的分子机制,从而导致精神运动激活增加。
