Lewis大鼠低遗传差异亚系的风险决策和冲动行为差异。

IF 1.6 4区 医学 Q3 BEHAVIORAL SCIENCES
Behavioral neuroscience Pub Date : 2023-08-01 Epub Date: 2023-04-27 DOI:10.1037/bne0000557
Daniel B K Gabriel, Anna E Liley, Hunter T Franks, Grace L Minnes, Monika Tutaj, Melinda R Dwinell, Tristan V de Jong, Robert W Williams, Megan K Mulligan, Hao Chen, Nicholas W Simon
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引用次数: 0

摘要

物质使用障碍(SUD)与一系列认知障碍有关,这些障碍会导致持续的药物寻求和复发。其中两种内在表型——SUD患者的风险决策和冲动性被放大,并因反复接触非法药物而增强。识别这些行为模式变异性背后的遗传因素对于早期识别、预防和治疗SUD易感个体至关重要。在这里,我们比较了Lewis大鼠LEW/NCrl和LEW/NHsd的两个完全自交系之间的风险决策和冲动的不同方面。我们对这两个子串进行了全基因组测序,以确定几乎所有相关的变体。我们观察到风险决策和冲动行为之间存在显著差异。相对于LEW/NHsd,LEW/NCrl子串在决策任务中接受更高的风险选择,在低反应率任务的差异强化中接受更大的过早反应率。这些表型差异在雌性中比雄性更明显。我们在40倍全基因组短阅读覆盖率下定义了这些子串之间总共约9000个多态性。大约一半的变体位于8号染色体的单个1.5Mb区域内,但没有影响蛋白质编码区域。相反,其他变体分布广泛,其中38种被预测会导致蛋白质编码变体。总之,Lewis大鼠的子串在冒险和冲动方面存在显著差异,只有少数易于映射的变体可能是因果关系。测序与降低复杂性的交叉应该能够识别多种复杂成瘾相关行为背后的一个或多个变体。(PsycInfo数据库记录(c)2023 APA,保留所有权利)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Divergent risky decision-making and impulsivity behaviors in Lewis rat substrains with low genetic difference.

Substance use disorder (SUD) is associated with a cluster of cognitive disturbances that engender vulnerability to ongoing drug seeking and relapse. Two of these endophenotypes-risky decision-making and impulsivity-are amplified in individuals with SUD and are augmented by repeated exposure to illicit drugs. Identifying genetic factors underlying variability in these behavioral patterns is critical for early identification, prevention, and treatment of SUD-vulnerable individuals. Here, we compared risky decision-making and different facets of impulsivity between two fully inbred substrains of Lewis rats-LEW/NCrl and LEW/NHsd. We performed whole genome sequencing of both substrains to identify almost all relevant variants. We observed substantial differences in risky decision-making and impulsive behaviors. Relative to LEW/NHsd, the LEW/NCrl substrain accepts higher risk options in a decision-making task and higher rates of premature responses in the differential reinforcement of low rates of responding task. These phenotypic differences were more pronounced in females than males. We defined a total of ∼9,000 polymorphisms between these substrains at 40× whole genome short-read coverage. Roughly half of variants are located within a single 1.5 Mb region of Chromosome 8, but none impact protein-coding regions. In contrast, other variants are widely distributed, and of these, 38 are predicted to cause protein-coding variants. In conclusion, Lewis rat substrains differ significantly in risk-taking and impulsivity and only a small number of easily mapped variants are likely to be causal. Sequencing combined with a reduced complexity cross should enable identification of one or more variants underlying multiple complex addiction-relevant behaviors. (PsycInfo Database Record (c) 2023 APA, all rights reserved).

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来源期刊
Behavioral neuroscience
Behavioral neuroscience 医学-行为科学
CiteScore
3.40
自引率
0.00%
发文量
51
审稿时长
6-12 weeks
期刊介绍: Behavioral Neuroscience publishes original research articles as well as reviews in the broad field of the neural bases of behavior.
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