Hall F Scott, Sora I, Uhl G R
Molecular Neurobiology Branch, NIDA-IRP, NIH, DHHS, Baltimore, MD, USA.
Neuropsychopharmacology. 2003 Apr;28(4):620-8. doi: 10.1038/sj.npp.1300070. Epub 2002 Sep 20.
Several lines of evidence suggest that monoaminergic systems, especially dopaminergic and serotoninergic systems, modulate ethanol consumption. Humans display significant differences in expression of the vesicular and plasma membrane monoamine transporters important for monoaminergic functions, including the vesicular monoamine transporter (VMAT2, SLC18A2) and dopamine transporter (DAT, SLC6A3). In addition, many ethanol effects differ by sex in both humans and animal models. Therefore, ethanol consumption and preference were compared in male and female wild-type mice, and knockout (KO) mice with deletions of genes for DAT and VMAT2. Voluntary ethanol (2-32% v/v) and water consumption were compared in two-bottle preference tests in wild-type (+/+) vs heterozygous VMAT2 KO mice (+/-) and in wild-type (+/+) vs heterozygous (+/-) or homozygous (-/-) DAT KO mice. Deletions of either the DAT or VMAT2 genes increased ethanol consumption in male KO mice, although these effects were highly dependent on ethanol concentration, while female DAT KO mice had higher ethanol preferences. Thus, lifetime reductions in the expression of either DAT or VMAT2 increase ethanol consumption, dependent on sex.
多条证据表明,单胺能系统,尤其是多巴胺能和5-羟色胺能系统,会调节乙醇消耗。人类在对单胺能功能至关重要的囊泡和质膜单胺转运体的表达上存在显著差异,包括囊泡单胺转运体(VMAT2,SLC18A2)和多巴胺转运体(DAT,SLC6A3)。此外,在人类和动物模型中,许多乙醇效应存在性别差异。因此,对雄性和雌性野生型小鼠以及缺失DAT和VMAT2基因的基因敲除(KO)小鼠的乙醇消耗和偏好进行了比较。在野生型(+/+)与杂合VMAT2基因敲除小鼠(+/-)以及野生型(+/+)与杂合(+/-)或纯合(-/-)DAT基因敲除小鼠的双瓶偏好试验中,比较了自愿乙醇(2-32% v/v)和水的消耗情况。DAT或VMAT2基因的缺失增加了雄性基因敲除小鼠的乙醇消耗,尽管这些效应高度依赖于乙醇浓度,而雌性DAT基因敲除小鼠对乙醇的偏好更高。因此,DAT或VMAT2表达的终生减少会增加乙醇消耗,这取决于性别。