Lee C M, Snyder S H
Proc Natl Acad Sci U S A. 1981 Aug;78(8):5250-4. doi: 10.1073/pnas.78.8.5250.
Neuronal uptake recognition sites in norepinephrine neurons have been labeled with the antidepressant [3H]desipramine. A high-affinity component of [3H]desipramine binding to rat cerebral cortex membranes is abolished selectively by 6-hydroxydopamine lesions, which destroy central catecholamine neurons. The high-affinity [3H]desipramine binding has a nanomolar affinity constant for desipramine and is inhibited by tricyclic antidepressants with potencies that correlate with their ability to inhibit the neuronal uptake of norepinephrine. [3H]Desipramine binding to the uptake sites is markedly stimulated by sodium, with potassium, lithium, and choline being much less effective. The ability to monitor norepinephrine neuronal uptake "receptors" in simple binding studies should permit a differential analysis of drug influences on the norepinephrine recognition site and the translocation mechanism. The regulation of [3H]desipramine binding by sodium may help clarify how sodium influences neurotransmitter uptake.
去甲肾上腺素能神经元中的神经元摄取识别位点已用抗抑郁药[3H]地昔帕明标记。[3H]地昔帕明与大鼠大脑皮层膜结合的高亲和力成分被6-羟基多巴胺损伤选择性消除,这种损伤会破坏中枢儿茶酚胺能神经元。[3H]地昔帕明的高亲和力结合对其具有纳摩尔亲和力常数,并且被三环类抗抑郁药抑制,其效力与其抑制去甲肾上腺素神经元摄取的能力相关。[3H]地昔帕明与摄取位点的结合受到钠的显著刺激,而钾、锂和胆碱的作用则小得多。在简单的结合研究中监测去甲肾上腺素神经元摄取“受体”的能力应允许对药物对去甲肾上腺素识别位点和转运机制的影响进行差异分析。钠对[3H]地昔帕明结合的调节可能有助于阐明钠如何影响神经递质摄取。