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首页> 外文期刊>Neuropharmacology >Selective inhibition of phosphodiesterase 10A impairs appetitive and aversive conditioning and incentive salience attribution
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Selective inhibition of phosphodiesterase 10A impairs appetitive and aversive conditioning and incentive salience attribution

机译:磷酸二酯酶10A的选择性抑制损害食欲和厌恶条件,并刺激显着性归因

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摘要

The pharmacological effect of the selective PDE10A inhibitor 2-[4-(1-methyl-4-pyridin-4-yl-1H-pyrazol-3-yl)-phenoxymethyl]-quinoline succinic acid (MP-10) on aversively and appetitively motivated behavior in C57BL/6J mice was examined. MP-10 dose-dependently impaired performance on a highly demanding reward schedule during appetitive conditioning. The compound further affected cue-based, but not contextual aversive conditioning. Finally, dose-dependent impaired performance in an instrumentally conditioned reinforcement (ICR) task was found. This suggests that the observed behavioral effects of MP-10 can be at least partially ascribed to impaired incentive salience attribution. MP-10 administration dose-dependently enhanced striatal expression of the immediate early gene Zif268, which suggest that MP-10 affects the studied motivated behaviors by enhancing PDE10A-regulated striatal signaling. Striatal signaling thus appears to be crucial in processes that control reward-motivated behavior in general, and incentive salience attribution in particular. Continued research will prove valuable towards a better understanding of psychopathologies that affect reward-motivated behaviors, such as drug addiction and schizophrenia.
机译:选择性PDE10A抑制剂2- [4-(1-甲基-4-吡啶-4--4-基-1H-吡唑-3-基)-苯氧基甲基]-喹啉琥珀酸(MP-10)的药理作用检查了C57BL / 6J小鼠的动机行为。在饮食调理过程中,MP-10剂量依赖性地损害了高要求奖励计划的性能。该化合物进一步影响基于提示的情境,但不影响上下文厌恶条件。最后,发现在仪器调节的加固(ICR)任务中剂量依赖性的性能下降。这表明观察到的MP-10的行为效应至少可以部分归因于动机显着性归因受损。 MP-10给药剂量依赖性地增强了立即早期基因Zif268的纹状体表达,这表明MP-10通过增强PDE10A调节的纹状体信号传导来影响研究的动机行为。因此,纹状体信号在控制奖励动机行为,尤其是奖励显着性归因的过程中似乎至关重要。继续进行的研究对于更好地理解影响奖励动机举的行为(例如吸毒成瘾和精神分裂症)的心理病理学将具有重要的价值。

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