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D1-多巴胺受体在工作记忆中的作用:向执行动眼延迟反应任务的恒河猴前额叶皮层局部注射多巴胺拮抗剂。

The role of D1-dopamine receptor in working memory: local injections of dopamine antagonists into the prefrontal cortex of rhesus monkeys performing an oculomotor delayed-response task.

作者信息

Sawaguchi T, Goldman-Rakic P S

机构信息

Section of Neurobiology, Yale University School of Medicine, New Haven, Connecticut 06510.

出版信息

J Neurophysiol. 1994 Feb;71(2):515-28. doi: 10.1152/jn.1994.71.2.515.

Abstract
  1. To examine the role of dopamine receptors in the prefrontal cortex (PFC) on working memory, we injected dopamine antagonists (SCH23390, SCH39166, haloperidol, sulpiride, and raclopride) locally into the dorsolateral PFC in two monkeys trained to perform an oculomotor delayed-response (ODR) task. In the ODR task, monkeys fixate a central spot on a cathode ray tube (CRT) monitor while a visual cue is briefly (300 ms) presented in one of several peripheral locations in the visual field. After a delay of 1.5-6 s, the fixation spot is turned off, instructing the monkey to move its eyes to the target location that had been indicated by the visuospatial cue before the delay. Each monkey also performed a control task in which the cue remained on during the delay period. In this task the monkey's response was sensory rather than memory guided. 2. Local intracerebral injection of the selective dopamine antagonists SCH23390 (10-80 micrograms) and SCH39166 (1-5 micrograms) and/or the nonselective dopamine antagonist haloperidol (10-100 micrograms) induced deficits in ODR task performance at a total of 22 sites in the dorsolateral PFC. The deficit was characterized by a decrease in the accuracy of the memory-guided saccade as well as an increase in the latency of the response. The deficit usually appeared within 1-3 min after the injection, reached a peak at 20-40 min, and recovered at 60-90 min. 3. Performance change was restricted to a few specific target locations, which varied with the injection site and were most often contralateral to the injection site. 4. The degree of impairment in the ODR task occasioned by the injection of the dopamine antagonists was sensitive to the duration of delay; longer delays were associated with larger decreases in the accuracy and delayed onset of the memory-guided saccade. 5. The deficit was dose dependent; higher doses induced larger errors and increases in the onset of the memory-guided saccade. 6. Dopamine antagonists did not affect performance on the control task, which required the same eye movements but was sensory guided. Thus, in the same experimental session in which ODR performance was impaired, the accuracy and the latency of the sensory-guided saccades were normal for every target location.(ABSTRACT TRUNCATED AT 400 WORDS)
摘要
  1. 为研究前额叶皮质(PFC)中的多巴胺受体在工作记忆中的作用,我们将多巴胺拮抗剂(SCH23390、SCH39166、氟哌啶醇、舒必利和雷氯必利)局部注射到两只经过训练以执行动眼延迟反应(ODR)任务的猴子的背外侧前额叶皮质中。在ODR任务中,猴子注视阴极射线管(CRT)显示器上的中央点,同时在视野中的几个周边位置之一短暂(300毫秒)呈现视觉提示。在1.5 - 6秒的延迟后,固定点关闭,指示猴子将眼睛移至延迟前视觉空间提示所指示的目标位置。每只猴子还执行了一项对照任务,其中提示在延迟期间保持显示。在这项任务中,猴子的反应是由感觉而非记忆引导的。2. 局部脑内注射选择性多巴胺拮抗剂SCH23390(10 - 80微克)和SCH39166(1 - 5微克)和/或非选择性多巴胺拮抗剂氟哌啶醇(10 - 100微克)在背外侧前额叶皮质的总共22个部位诱导了ODR任务表现的缺陷。该缺陷的特征是记忆引导扫视的准确性降低以及反应潜伏期增加。该缺陷通常在注射后1 - 3分钟内出现,在20 - 40分钟达到峰值,并在60 - 90分钟恢复。3. 性能变化仅限于几个特定的目标位置,这些位置随注射部位而变化,并且最常与注射部位对侧。4. 注射多巴胺拮抗剂引起的ODR任务中的损伤程度对延迟持续时间敏感;更长的延迟与记忆引导扫视的准确性更大降低和延迟发作相关。5. 缺陷是剂量依赖性的;更高剂量会导致更大的误差和记忆引导扫视发作的增加。6. 多巴胺拮抗剂不影响对照任务的表现,对照任务需要相同的眼球运动但由感觉引导。因此,在ODR表现受损的同一实验环节中,每个目标位置的感觉引导扫视的准确性和潜伏期都是正常的。(摘要截断于400字)

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