慢性吗啡给药后阿片受体异源二聚体丰度增加。
Increased abundance of opioid receptor heteromers after chronic morphine administration.
机构信息
Department of Pharmacology and Systems Therapeutics, Mount Sinai School of Medicine, New York, NY 10029, USA.
出版信息
Sci Signal. 2010 Jul 20;3(131):ra54. doi: 10.1126/scisignal.2000807.
Abstract
The mu and delta types of opioid receptors form heteromers that exhibit pharmacological and functional properties distinct from those of homomeric receptors. To characterize these complexes in the brain, we generated antibodies that selectively recognize the mu-delta heteromer and blocked its in vitro signaling. With these antibodies, we showed that chronic, but not acute, morphine treatment caused an increase in the abundance of mu-delta heteromers in key areas of the central nervous system that are implicated in pain processing. Because of its distinct signaling properties, the mu-delta heteromer could be a therapeutic target in the treatment of chronic pain and addiction.
摘要
μ 和 δ 型阿片受体形成杂二聚体,表现出与同型受体不同的药理学和功能特性。为了在大脑中表征这些复合物,我们生成了选择性识别 μ-δ 杂二聚体并阻断其体外信号转导的抗体。使用这些抗体,我们表明慢性而非急性吗啡处理会导致与疼痛处理有关的中枢神经系统关键区域中 μ-δ 杂二聚体的丰度增加。由于其独特的信号转导特性,μ-δ 杂二聚体可能成为治疗慢性疼痛和成瘾的治疗靶点。
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