首页> 外文期刊>Behavioural Brain Research: An International Journal >Group I metabotropic glutamate receptor antagonists impair discriminability of reinforcer magnitude, but not risky choice, in a probability-discounting task
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Group I metabotropic glutamate receptor antagonists impair discriminability of reinforcer magnitude, but not risky choice, in a probability-discounting task

机译:概率折扣任务中,Ⅰ组代谢谷氨酸受体拮抗剂损害了增强剂幅度的可怜,但不能有风险的选择

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The glutamatergic system has been identified as an important mediator of risky choice. However, previous studies have focused primarily on ionotropic glutamate receptors (e.g., NMDA receptors). Little research has examined the contribution of metabotropic glutamate receptors (mGluRs) on risky choice. The goal of the current experiment was to determine the effects of mGluR(1) and mGluR(5) antagonism on risky choice as assessed in probability discounting (PD). Male Sprague Dawley rats (n = 24) were trained in PD, in which consistently choosing a large, probabilistic reward (LR) reflects risky choice. For half of the rats, the odds against (OA) receiving the LR increased across blocks of trials, whereas the OA decreased across the session for half of the rats. Following training, rats received injections of the mGluR(1) antagonist JNJ 16,259,685 (JNJ; 0, 0.1, 0.3, or 1.0 mg/kg; i.p) and the mGluR(5 )antagonist MTEP (0, 1.0, 3.0, or 10.0 mg/kg; i.p.). Regardless of which schedule was used, JNJ and MTEP decreased preference for the LR when its delivery was guaranteed. In contrast to delay discounting, in which blocking the mGluR(1) has been shown to alter impulsive choice, these results show that the Group I mGluR family does not selectively alter risky choice. Instead, blocking these receptors appears to impair discriminability of reinforcers of varying magnitudes in PD.
机译:谷氨酸系统已被确定为风险选择的重要调解员。然而,先前的研究主要集中在离子淋谷氨酸受体(例如NMDA受体)上。较少的研究已经研究了代谢谷氨酸受体(MGLURURS)对风险选择的贡献。目前实验的目的是确定MgluR(1)和MgluR(5)对危险选择的影响,如概率折扣(PD)评估。雄性Sprague Dawley大鼠(N = 24)在PD中培训,其中一致地选择大型概率奖励(LR)反映了风险的选择。对于一半的大鼠来说,接受LR的赔率(OA)横跨试验块增加,而OA在会议上减少了一半的大鼠。在培训之后,大鼠接受了MGLUR(1)拮抗剂JNJ 16,259,685(JNJ; 0,0.1,0.3或1.0mg / kg; IP)和MGLUR(5)拮抗剂MTEP(0,1.0,3.0或10.0mg / kg; IP)。无论使用哪个计划,当保证其交付时,JNJ和MTEP就会减少对LR的偏好。与延迟折扣相比,封闭MGLUR(1)已经显示出改变冲动的选择,这些结果表明,I MGLUR系列没有选择性地改变风险的选择。相反,阻断这些受体似乎损害了Pd中改变幅度的增强剂的可怜。

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