Lowing Jennifer L, Susick Laura L, Caruso James P, Provenzano Anthony M, Raghupathi Ramesh, Conti Alana C
1 John D. Dingell VA Medical Center, Wayne State University School of Medicine , Detroit, Michigan.
J Neurotrauma. 2014 Oct 15;31(20):1700-10. doi: 10.1089/neu.2013.3286. Epub 2014 Sep 2.
Altered alcohol consumption patterns after traumatic brain injury (TBI) can lead to significant impairments in TBI recovery. Few preclinical models have been used to examine alcohol use across distinct phases of the post-injury period, leaving mechanistic questions unanswered. To address this, the aim of this study was to describe the histological and behavioral outcomes of a noncontusive closed-head TBI in the mouse, after which sensitivity to and consumption of alcohol were quantified, in addition to dopaminergic signaling markers. We hypothesized that TBI would alter alcohol consumption patterns and related signal transduction pathways that were congruent to clinical observations. After midline impact to the skull, latency to right after injury, motor deficits, traumatic axonal injury, and reactive astrogliosis were evaluated in C57BL/6J mice. Amyloid precursor protein (APP) accumulation was observed in white matter tracts at 6, 24, and 72 h post-TBI. Increased intensity of glial fibrillary acidic protein (GFAP) immunoreactivity was observed by 24 h, primarily under the impact site and in the nucleus accumbens, a striatal subregion, as early as 72 h, persisting to 7 days, after TBI. At 14 days post-TBI, when mice were tested for ethanol sensitivity after acute high-dose ethanol (4 g/kg, intraperitoneally), brain-injured mice exhibited increased sedation time compared with uninjured mice, which was accompanied by deficits in striatal dopamine- and cAMP-regulated neuronal phosphoprotein, 32 kDa (DARPP-32) phosphorylation. At 17 days post-TBI, ethanol intake was assessed using the Drinking-in-the-Dark paradigm. Intake across 7 days of consumption was significantly reduced in TBI mice compared with sham controls, paralleling the reduction in alcohol consumption observed clinically in the initial post-injury period. These data demonstrate that TBI increases sensitivity to ethanol-induced sedation and affects downstream signaling mediators of striatal dopaminergic neurotransmission while altering ethanol consumption. Examining TBI effects on ethanol responsitivity will improve our understanding of alcohol use post-TBI in humans.
创伤性脑损伤(TBI)后饮酒模式的改变会导致TBI恢复出现显著障碍。很少有临床前模型被用于研究损伤后不同阶段的酒精使用情况,这使得一些机制性问题仍未得到解答。为了解决这个问题,本研究的目的是描述小鼠非挫伤性闭合性头部TBI的组织学和行为学结果,之后除了对多巴胺能信号标记物进行量化外,还对酒精敏感性和酒精消耗量进行了测定。我们假设TBI会改变与临床观察结果一致的酒精消费模式和相关信号转导途径。在对C57BL/6J小鼠的颅骨进行中线撞击后,评估了损伤后右侧翻身潜伏期、运动功能缺陷、创伤性轴索损伤和反应性星形胶质细胞增生。在TBI后6、24和72小时,在白质束中观察到淀粉样前体蛋白(APP)的积累。早在TBI后72小时,在撞击部位下方和伏隔核(纹状体的一个亚区域)观察到胶质纤维酸性蛋白(GFAP)免疫反应性强度增加,持续到7天。在TBI后14天,当对小鼠进行急性高剂量乙醇(4克/千克,腹腔注射)后的乙醇敏感性测试时,与未受伤的小鼠相比,脑损伤小鼠的镇静时间增加,同时伴有纹状体中多巴胺和cAMP调节的神经元磷蛋白32 kDa(DARPP-32)磷酸化的缺陷。在TBI后17天,使用黑暗中饮水范式评估乙醇摄入量。与假手术对照组相比,TBI小鼠7天的摄入量显著减少,这与损伤后初期临床上观察到的酒精消耗量减少情况相似。这些数据表明,TBI增加了对乙醇诱导的镇静的敏感性,影响纹状体多巴胺能神经传递的下游信号介质,同时改变乙醇消耗量。研究TBI对乙醇反应性的影响将有助于我们更好地理解人类TBI后的酒精使用情况。
