Alsiö J, Nilsson S R O, Gastambide F, Wang R A H, Dam S A, Mar A C, Tricklebank M, Robbins T W
Department of Psychology, University of Cambridge, Cambridge, CB2 3EB, UK.
Behavioural and Clinical Neuroscience Institute, University of Cambridge, Cambridge, CB2 3EB, UK.
Psychopharmacology (Berl). 2015 Nov;232(21-22):4017-31. doi: 10.1007/s00213-015-3963-5. Epub 2015 May 26.
Reversal learning requires associative learning and executive functioning to suppress non-adaptive responding. Reversal-learning deficits are observed in e.g. schizophrenia and obsessive-compulsive disorder and implicate neural circuitry including the orbitofrontal cortex (OFC). Serotonergic function has been strongly linked to visual reversal learning in humans and experimental animals but less is known about which receptor subtypes are involved.
The objectives of the study were to test the effects of systemic and intra-OFC 5-HT2C-receptor antagonism on visual reversal learning in rats and assess the psychological mechanisms underlying these effects within novel touchscreen paradigms.
In experiments 1-2, we used a novel 3-stimulus task to investigate the effects of 5-HT2C-receptor antagonism through SB 242084 (0.1, 0.5 and 1.0 mg/kg i.p.) cross-site. Experiment 3 assessed the effects of SB 242084 in 2-choice reversal learning. In experiment 4, we validated a novel touchscreen serial visual reversal task suitable for neuropharmacological microinfusions by baclofen-/muscimol-induced OFC inactivation. In experiment 5, we tested the effect of intra-OFC SB 242084 (1.0 or 3.0 μg/side) on performance in this task.
In experiments 1-3, SB 242084 reduced early errors but increased late errors to criterion. In experiment 5, intra-OFC SB 242084 reduced early errors without increasing late errors in a reversal paradigm validated as OFC dependent (experiment 4).
Intra-OFC 5-HT2C-receptor antagonism decreases perseveration in novel touchscreen reversal-learning paradigms for the rat. Systemic 5-HT2C-receptor antagonism additionally impairs late learning-a robust effect observed cross-site and potentially linked to impulsivity. These conclusions are discussed in terms of neural mechanisms underlying reversal learning and their relevance to psychiatric disorders.
反转学习需要联想学习和执行功能来抑制非适应性反应。在精神分裂症和强迫症等疾病中观察到反转学习缺陷,这涉及包括眶额皮质(OFC)在内的神经回路。血清素能功能与人类和实验动物的视觉反转学习密切相关,但对于涉及哪些受体亚型知之甚少。
本研究的目的是测试全身和OFC内5-HT2C受体拮抗作用对大鼠视觉反转学习的影响,并在新型触摸屏范式中评估这些影响背后的心理机制。
在实验1-2中,我们使用一种新型的三刺激任务,通过腹腔注射SB 242084(0.1、0.5和1.0mg/kg)跨部位研究5-HT2C受体拮抗作用的影响。实验3评估了SB 242084在二选一反转学习中的作用。在实验4中,我们通过巴氯芬/蝇蕈醇诱导的OFC失活验证了一种适用于神经药理学微量注射的新型触摸屏连续视觉反转任务。在实验5中,我们测试了OFC内注射SB 242084(1.0或3.0μg/侧)对该任务表现的影响。
在实验1-3中,SB 242084减少了早期错误,但增加了达到标准的晚期错误。在实验5中,在被验证为依赖OFC的反转范式中,OFC内注射SB 242084减少了早期错误,而没有增加晚期错误(实验4)。
OFC内5-HT2C受体拮抗作用可减少大鼠在新型触摸屏反转学习范式中的持续性。全身5-HT2C受体拮抗作用还会损害晚期学习——这是一种在跨部位观察到的强烈效应,可能与冲动性有关。这些结论将根据反转学习的神经机制及其与精神疾病的相关性进行讨论。
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