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乙醇对运动活动影响的双向选择育种:通过第35代选择对快速和慢速小鼠的特征描述

Bidirectional selective breeding for ethanol effects on locomotor activity: characterization of FAST and SLOW mice through selection generation 35.

作者信息

Shen E H, Harland R D, Crabbe J C, Phillips T J

机构信息

Department of Medical Psychology, Oregon Health Sciences University, Portland, USA.

出版信息

Alcohol Clin Exp Res. 1995 Oct;19(5):1234-45. doi: 10.1111/j.1530-0277.1995.tb01606.x.

DOI:10.1111/j.1530-0277.1995.tb01606.x
PMID:8561296
Abstract

Increased recognition of the advantages of genetic animal models has led to heightened interest in their use and development. A replicated bidirectional selective breeding project has produced lines of mice that differ in their locomotor responses to 2.0 g/kg ethanol. FAST-1 and FAST-2 mice are highly stimulated by ethanol (EtOH), whereas SLOW-1 and SLOW-2 mice are either not affected or respond with locomotor depression. Current heritability estimates indicate that approximately 6-8% of the response variance in the FAST lines and 2-10% of the response variance in the SLOW lines is of additive genetic origin. Little systematic response to selection has occurred in recent generations, which implies that the limits of selection have been reached. Analysis of saline activity over 35 generations of selection indicates that baseline activities have not changed during the course of selection in three of the lines, whereas baseline activity of FAST-1 mice has increased slightly. In EtOH dose-response studies (0.5-3.0 g/kg), FAST mice had biphasic dose-response curves, whereas the locomotor activity of SLOW mice was either unaffected or depressed by all doses of EtOH. In addition, FAST mice spent more time in motion, traveled farther per movement, traversed greater distances in the center of the test chamber, and ambulated more quickly than SLOW mice when given EtOH. FAST and SLOW mice differed in EtOH clearance rates; however, the differences were slight relative to the large difference in locomotor response. We encourage the use of FAST and SLOW mice to investigate neurophysiological factors underlying sensitivity to the behavioral effects of EtOH, with a view to further testing of the postulated homology between locomotor stimulant effects and addiction potential of drugs of abuse.

摘要

对基因动物模型优势的更多认识引发了人们对其使用和开发的浓厚兴趣。一个重复的双向选择性育种项目培育出了对2.0 g/kg乙醇的运动反应不同的小鼠品系。FAST-1和FAST-2小鼠受到乙醇(EtOH)的强烈刺激,而SLOW-1和SLOW-2小鼠要么不受影响,要么表现出运动抑制。目前的遗传力估计表明,FAST品系中约6-8%的反应方差以及SLOW品系中2-10%的反应方差源于加性遗传。近几代对选择几乎没有系统性反应,这意味着已达到选择极限。对35代选择过程中的生理盐水活动分析表明,其中三个品系在选择过程中基线活动没有变化,而FAST-1小鼠的基线活动略有增加。在乙醇剂量反应研究(0.5-3.0 g/kg)中,FAST小鼠具有双相剂量反应曲线,而SLOW小鼠的运动活动要么不受所有剂量乙醇的影响,要么受到抑制。此外,给予乙醇时,FAST小鼠运动时间更长,每次移动距离更远,在测试室中心走过的距离更大,行走速度比SLOW小鼠更快。FAST和SLOW小鼠在乙醇清除率上存在差异;然而,相对于运动反应的巨大差异,这些差异很小。我们鼓励使用FAST和SLOW小鼠来研究对乙醇行为效应敏感性的神经生理因素,以便进一步测试运动刺激效应与滥用药物成瘾潜力之间假定的同源性。

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