mPFC catecholamines modulate attentional capture by appetitive distracters and attention to time in a peak-interval procedure in rats.

IF 1.6 4区 医学 Q3 BEHAVIORAL SCIENCES Behavioral neuroscience Pub Date : 2022-10-01 Epub Date: 2022-07-14 DOI:10.1037/bne0000528
Catalin V Buhusi, Alexander R Matthews, Mona Buhusi
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引用次数: 1

Abstract

The behavioral and neural mechanisms by which distracters delay interval timing behavior are currently unclear. Distracters delay timing in a considerable dynamic range: Some distracters have no effect on timing ("run"), whereas others seem to "stop" timing; some distracters restart ("reset") the entire timing mechanisms at their offset, whereas others seem to capture attentional resources long after their termination ("over-reset"). While the run-reset range of delays is accounted for by the Time-Sharing Hypothesis (Buhusi, 2003, 2012), the behavioral and neural mechanisms of "over-resetting" are currently uncertain. We investigated the role of novelty (novel/familiar) and significance (consequential/inconsequential) in the time-delaying effect of distracters and the role of medial prefrontal cortex (mPFC) catecholamines by local infusion of norepinephrine-dopamine reuptake inhibitor (NDRI) nomifensine in a peak-interval (PI) procedure in rats. Results indicate differences in time delay between groups, suggesting a role for both novelty and significance: inconsequential, familiar distracters "stopped" timing, novel distracters "reset" timing, whereas appetitively conditioned distracters "over-reset" timing. mPFC infusion of nomifensine modulated attentional capture by appetitive distracters in a "U"-shaped fashion, reduced the delay after novel distracters, but had no effects after inconsequential, familiar distracters. These results were not due to nomifensine affecting either timing accuracy, precision, or peak response rate. Results may help elucidate the behavioral and physiological mechanisms underlying interval timing and attention to time and may contribute to developing new treatment strategies for disorders of attention. (PsycInfo Database Record (c) 2022 APA, all rights reserved).

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mPFC儿茶酚胺通过食欲干扰物调节大鼠的注意力捕获,并在峰值间隔过程中调节对时间的注意力。
分心者延迟间隔时间行为的行为和神经机制目前尚不清楚。分心者在相当大的动态范围内延迟时间:一些分心者对时间没有影响(“跑”),而另一些则似乎“停止”了时间;一些干扰源在其偏移处重新启动(“重置”)整个时间机制,而另一些干扰源似乎在其终止后很长一段时间才捕获注意力资源(“过度重置”)。虽然时间共享假说(Buhusi,20032012)解释了延迟的运行重置范围,但“过度重置”的行为和神经机制目前尚不确定。我们通过在大鼠峰值间期(PI)程序中局部输注去甲肾上腺素-多巴胺再摄取抑制剂(NDRI)诺米芬,研究了新颖性(新颖/熟悉)和显著性(重要/无关紧要)在干扰物的时间延迟效应中的作用,以及内侧前额叶皮层(mPFC)儿茶酚胺的作用。结果表明,各组之间的时间延迟存在差异,这表明了新颖性和显著性的作用:无关紧要的、熟悉的干扰物“停止”时间,新颖的干扰器“重置”时间,而食欲条件干扰物则“过度重置”时间。mPFC输注诺米芬嗪以“U”型方式调节食欲干扰物的注意力捕获,减少了新型干扰物后的延迟,但在无关紧要的、熟悉的干扰物之后没有影响。这些结果并不是由于诺芬嗪影响了计时精度、精度或峰值响应率。研究结果可能有助于阐明间隔时间和注意力对时间的潜在行为和生理机制,并可能为开发新的注意力障碍治疗策略做出贡献。(PsycInfo数据库记录(c)2022 APA,保留所有权利)。
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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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