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首页> 外文期刊>European Journal of Pharmacology: An International Journal >Release studies with rat brain cortical synaptosomes indicate that tramadol is a 5-hydroxytryptamine uptake blocker and not a 5-hydroxytryptamine releaser.
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Release studies with rat brain cortical synaptosomes indicate that tramadol is a 5-hydroxytryptamine uptake blocker and not a 5-hydroxytryptamine releaser.

机译:用大鼠脑皮质突触小体进行的释放研究表明,曲马多是5-羟​​色胺摄取的阻断剂,而不是5-羟色胺释放剂。

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摘要

Tramadol is a centrally acting opioid analgesic whose mechanism of action could also involve an increase in central serotoninergic transmission. Thus, tramadol inhibits synaptosomal serotonin (5-hydroxytryptamine, 5-HT) reuptake and induces tritium release from [3H]5-HT-preloaded slices. We investigated the effect of (+/-)-tramadol in release studies with superfused rat brain cortex synaptosomes preloaded with [3H]5-HT. Tramadol had no releasing effect up to 30 microM, whereas at 10 microM tramadol significantly inhibited by 45% D-fenfluramine-induced [3H]5-HT release. At 100 microM, tramadol showed a slight releasing effect in the absence or in the presence of pargyline, which was not augmented in synaptosomes pre-exposed to Ro 04-1284 (2-ethyl-1,3,4,6,7,11b-hexahydro-3-isobutyl-9,10-dimethoxy-2H-benzo [a]quinolizin-2-ol hydrochloride), a reserpine-like compound that enhances cytoplasmic 5-HT levels. In summary, (+/-)-tramadol behaved as a classical 5-HT uptake blocker (like citalopram) and not as a substrate of the 5-HT carrier with indirect 5-HT mimetic properties (like D-fenfluramine).
机译:曲马多是一种中枢性阿片类镇痛药,其作用机理也可能涉及中枢5-羟色胺能传递的增加。因此,曲马多抑制突触体5-羟色胺(5-羟色胺,5-HT)的再摄取并诱导[从[3H] 5-HT预载片中释放。我们在预混有[3H] 5-HT的超融合大鼠脑皮质突触体的释放研究中研究了(+/-)-曲马多的作用。曲马多直到30 microM都没有释放作用,而在10 microM时,曲马多显着抑制了45%D-芬氟拉明诱导的[3H] 5-HT释放。在100 microM时,曲马多在不存在或存在pargyline的情况下显示出轻微的释放作用,而在预先暴露于Ro 04-1284(2-乙基-1,3,4,6,7,11b -六氢-3-异丁基-9,10-二甲氧基-2H-苯并[a]喹诺嗪-2-醇盐酸盐),类利血平的化合物,可提高细胞质5-HT水平。总之,(+/-)-曲马多表现为经典的5-HT吸收阻滞剂(如西酞普兰),而不是具有间接5-HT模仿性质的5-HT载体的底物(如D-芬氟拉明)。

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