Littleton John, Zieglgänsberger Walter
Department of Molecular and Biomedical Pharmacology, University of Kentucky, Lexington, KY 40546-0236, USA.
Am J Addict. 2003;12(s1):s3-s11. doi: 10.1111/j.1521-0391.2003.tb00492.x.
Naltrexone and acamprosate may ultimately prove to be useful additions to pharmacotherapy for alcoholism by reducing relapse. Naltrexone is a relatively selective competitive antagonist at mu-opioid receptors, and this activity may explain its anti-relapse action either because endogenous opioids are involved in the positively reinforcing effects of alcohol and/or because these same transmitters are involved in the conditioned anticipation of these effects. In contrast, the pharmacology of acamprosate is still poorly understood. This is not surprising because it is a small flexible molecule with similarities to several neuro-active amino acids and is used in high doses. All these factors suggest that it may have multiple actions. Currently, the best explanation for the effects of acamprosate seems to be that it inhibits the glutamatergic transmitter system involved in both the negative reinforcing effects of alcohol and the conditioned "pseudo-withdrawal" that may be important in cue-induced relapse.
纳曲酮和阿坎酸最终可能被证明是通过减少复发来有效辅助酒精中毒药物治疗的药物。纳曲酮是一种相对选择性的μ-阿片受体竞争性拮抗剂,这种活性可能解释了它的抗复发作用,原因可能是内源性阿片类物质参与了酒精的正性强化作用,和/或因为这些相同的递质参与了对这些作用的条件性预期。相比之下,阿坎酸的药理作用仍知之甚少。这并不奇怪,因为它是一个小的柔性分子,与几种神经活性氨基酸相似,且使用剂量很高。所有这些因素表明它可能有多种作用。目前,对阿坎酸作用的最佳解释似乎是它抑制了谷氨酸能递质系统,该系统既参与了酒精的负性强化作用,也参与了条件性“假性戒断”,而这在提示诱导的复发中可能很重要。