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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Cyclic AMP AMP ‐producing chemogenetic activation of indirect pathway striatal projection neurons and the downstream effects on the globus pallidus and subthalamic nucleus in freely moving mice
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Cyclic AMP AMP ‐producing chemogenetic activation of indirect pathway striatal projection neurons and the downstream effects on the globus pallidus and subthalamic nucleus in freely moving mice

机译:循环amp amp-在自由移动小鼠中对间接途径纹状体投影神经元和下游效应的循环amp amps促进了间接途径纹状体投影神经元的下游效应

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Abstract The indirect pathway striatal medium spiny projection neurons ( iMSN s) are critical to motor and cognitive brain functions. These neurons express a high level of cAMP ‐increasing adenosine A2a receptors. However, the potential effects of cAMP production on iMSN spiking activity have not been established, and recording identified iMSN s in freely moving animals is challenging. Here, we show that in the transgenic mice expressing cAMP ‐producing G protein G s ‐coupled designer receptor exclusively activated by designer drug (Gs‐ DREADD ) in iMSN s, the baseline spike firing in MSN s is normal, indicating DREADD expression does not affect the normal physiology of these neurons. Intraperitoneal injection of the DREADD agonist clozapine‐N‐oxide ( CNO ; 2.5?mg/kg) increased the spike firing in 50% of the recorded MSN s. However, CNO did not affect MSN firing in Gs‐ DREADD ‐negative mice. We also found that CNO injection inhibited the spike firing of globus pallidus external segment ( GP e) neurons in Gs‐ DREADD ‐positive mice, further indicating CNO excitation of iMSN s. Temporally coincident with these effects on spiking firing in the indirect pathway, CNO injection selectively inhibited locomotion in D2 Gs‐ DREADD mice. Taken together, our results strongly suggest that cAMP production in iMSN s can increase iMSN spiking activity and cause motor inhibition, thus addressing a long‐standing question about the cellular functions of the cAMP ‐producing adenosine A2a receptors in iMSN s. Cover Image for this issue: doi: 10.1111/jnc.14181 .
机译:摘要间接途径纹纹培养型多刺的凸起神经元(IMSN S)对电动机和认知脑功能至关重要。这些神经元表达了高水平的营养营养腺苷A2A受体。然而,营地生产对IMSN尖峰活动的潜在影响尚未建立,并且在自由移动的动物中识别IMSN S的录音是具有挑战性的。在这里,我们表明,在表达CAMP的转基因小鼠中,在IMSN S中专门由设计者药物(GS-DREADD)分开激活的G蛋白G的G蛋白G的S-Cubupled设计者受体,MSN S中的基线尖峰烧制是正常的,表明Dreadd表达没有影响这些神经元的正常生理学。腹膜内注射Dreadd激动剂氯氮平-N-氧化物(CNO; 2.5?Mg / kg)在记录的MSN S中的50%中增加了尖峰烧制。然而,CNO在GS-DREADD-Negative小鼠中没有影响MSN射击。我们还发现,CNO注射抑制GS-DREADD - 阳性小鼠中Globus Pallidus外部段(GP E)神经元的尖峰烧制,进一步表明IMSN S的CNO激发。在间接途径中对尖刺射击的这些作用进行时间逐步一致,CNO注射选择性地抑制D2 GS-Dreadd小鼠的运动。我们的结果强烈建议,IMSN S中的营地生产可以增加IMSN尖峰活动并导致电机抑制,从而解决了关于CAMP的蜂窝状功能的长期问题 - 在IMSN S中发挥腺苷A2A受体。此问题的封面图像:DOI:10.1111 / JNC.14181。

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