Mergy Marc A, Gowrishankar Raajaram, Davis Gwynne L, Jessen Tammy N, Wright Jane, Stanwood Gregg D, Hahn Maureen K, Blakely Randy D
Departments of Pharmacology, Vanderbilt University School of Medicine, Nashville, TN, USA.
Department of Medicine, Vanderbilt University School of Medicine, Nashville, TN, USA.
Neurochem Int. 2014 Jul;73:56-70. doi: 10.1016/j.neuint.2013.11.009. Epub 2013 Dec 8.
Alterations in dopamine (DA) signaling underlie the most widely held theories of molecular and circuit level perturbations that lead to risk for attention-deficit hyperactivity disorder (ADHD). The DA transporter (DAT), a presynaptic reuptake protein whose activity provides critical support for DA signaling by limiting DA action at pre- and postsynaptic receptors, has been consistently associated with ADHD through pharmacological, behavioral, brain imaging and genetic studies. Currently, the animal models of ADHD exhibit significant limitations, stemming in large part from their lack of construct validity. To remedy this situation, we have pursued the creation of a mouse model derived from a functional nonsynonymous variant in the DAT gene (SLC6A3) of ADHD probands. We trace our path from the identification of these variants to in vitro biochemical and physiological studies to the production of the DAT Val559 mouse model. We discuss our initial findings with these animals and their promise in the context of existing rodent models of ADHD.
多巴胺(DA)信号传导的改变是导致注意力缺陷多动障碍(ADHD)风险的分子和电路水平扰动的最广泛接受的理论基础。DA转运体(DAT)是一种突触前再摄取蛋白,其活性通过限制DA在突触前和突触后受体上的作用为DA信号传导提供关键支持,通过药理学、行为学、脑成像和遗传学研究,它一直与ADHD相关。目前,ADHD的动物模型存在显著局限性,这在很大程度上源于它们缺乏建构效度。为了纠正这种情况,我们致力于创建一种小鼠模型,该模型源自ADHD先证者DAT基因(SLC6A3)中的功能性非同义变体。我们追踪了从鉴定这些变体到体外生化和生理学研究,再到生产DAT Val559小鼠模型的过程。我们讨论了对这些动物的初步研究结果以及它们在现有ADHD啮齿动物模型背景下的前景。