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首页> 外文期刊>The Journal of Physiology >Melanocortins and agouti-related protein modulate the excitability of two arcuate nucleus neuron populations by alteration of resting potassium conductances.
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Melanocortins and agouti-related protein modulate the excitability of two arcuate nucleus neuron populations by alteration of resting potassium conductances.

机译:黑皮质素和刺骨相关蛋白通过改变静息钾电导率来调节两个弓形核神经元群体的兴奋性。

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摘要

The hypothalamic melanocortin system is crucial for the control of appetite and body weight. Two of the five melanocortin receptors, MC3R and MC4R are involved in hypothalamic control of energy homeostasis, with the MC4R having the major influence. It is generally thought that the main impact of the melanocortin system on hypothalamic circuits is external to the arcuate nucleus, and that any effect locally in the arcuate nucleus is inhibitory on proopiomelanocortin-expressing (POMC) neurons. In contrast, using current- and voltage-clamp recordings from identified neurons, we demonstrate that MC3R and MC4R agonists depolarize arcuate POMC neurons and a separate arcuate neuronal population identified by the rat insulin 2 promoter (RIPCre) transgene expression. Furthermore, the endogenous MC3R and MC4R antagonist, agouti-related protein (AgRP), hyperpolarizes POMC and RIPCre neurons in the absence of melanocortin agonist, consistent with inverse agonism at the MC4R. A decreased transient outward (I(A)) potassium conductance, and to a lesser extent the inward rectifier (K(IR)) conductance, underlies neuronal depolarization, whereas an increase in I(A) mediates AgRP-induced hyperpolarization. Accordingly, POMC and RIPCre neurons may be targets for peptide transmitters that are possibly released locally from AgRP-expressing and POMC neurons in the arcuate nucleus, adding further previously unappreciated complexity to the arcuate system.
机译:下丘脑的黑皮质素系统对于控制食欲和体重至关重要。五个黑皮质素受体中的两个,MC3R和MC4R参与下丘脑能量稳态的控制,其中MC4R的影响最大。通常认为,黑皮质素系统对下丘脑回路的主要影响是弓形核的外部,并且弓形核中局部的任何作用都抑制了表达proopiomelanocortin(POMC)的神经元。相比之下,使用来自已识别神经元的电流钳位和电压钳位记录,我们证明MC3R和MC4R激动剂使弓形POMC神经元和大鼠胰岛素2启动子(RIPCre)转基因表达所鉴定的单独弓形神经元群体去极化。此外,在不存在黑皮质素激动剂的情况下,内源性MC3R和MC4R拮抗剂刺鼠相关蛋白(AgRP)使POMC和RIPCre神经元超极化,这与MC4R的反向激动作用一致。瞬态向外(I(A))钾电导降低,而向内整流器(K(IR))电导在较小程度上是神经元去极化的基础,而I(A)的增加介导了AgRP诱导的超极化。因此,POMC和RIPCre神经元可能是可能从弓形核表达AgRP和POMC神经元局部释放的肽递质的靶标,从而进一步增加了弓形系统以前未曾意识到的复杂性。

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