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Fast and Slow Oscillations Recruit Molecularly-Distinct Subnetworks of Lateral Hypothalamic Neurons In Situ

机译:快速和慢速振荡在原位招募下丘脑外侧神经元的分子独特子网络。

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摘要

Electrical signals generated by molecularly-distinct classes of lateral hypothalamus (LH) neurons have distinct physiological consequences. For example, LH orexin neurons promote net body energy expenditure, while LH non-orexin neurons [VGAT, melanin-concentrating hormone (MCH)] drive net energy conservation. Appropriate switching between such physiologically-opposing LH outputs is traditionally thought to require cell-type-specific chemical modulation of LH firing. However, it was recently found that, in vivo, the LH neurons are also physiologically exposed to electrical oscillations of different frequency bands. The role of the different physiological oscillation frequencies in firing of orexin vs non-orexin LH neurons remains unknown. Here, we used brain-slice whole-cell patch-clamp technology to target precisely-defined oscillation waveforms to individual molecularly-defined classes LH cells (orexin, VGAT, MCH, GAD65), while measuring the action potential output of the cells. By modulating the frequency of sinusoidal oscillatory input, we found that high-frequency oscillations (γ, ≈30–200 Hz) preferentially silenced the action potential output orexinLH cells. In contrast, low frequencies (δ-θ, ≈0.5–7 Hz) similarly permitted outputs from different LH cell types. This differential control of orexin and non-orexin cells by oscillation frequency was mediated by cell-specific, impedance-unrelated resonance mechanisms. These results substantiate electrical oscillations as a novel input modality for cell-type-specific control of LH firing, which offers an unforeseen way to control specific cell ensembles within this highly heterogeneous neuronal cluster.
机译:下丘脑外侧(LH)神经元的分子区分类产生的电信号具有明显的生理后果。例如,LH食欲素神经元促进身体净能量消耗,而LH非食欲神经元[VGAT,黑色素浓缩激素(MCH)]推动净能量守恒。传统上,在这样的生理上相反的LH输出之间进行适当的切换需要LH点火的细胞类型特定化学调制。然而,最近发现,在体内,LH神经元在生理上也暴露于不同频带的电振荡。不同的生理振荡频率在食欲素与非食欲素LH神经元放电中的作用仍然未知。在这里,我们使用脑切片全细胞膜片钳技术将精确定义的振荡波形定位到单个分子定义的LH细胞(毒素,VGAT,MCH,GAD65),同时测量细胞的动作电位输出。通过调制正弦振荡输入的频率,我们发现高频振荡(γ,≈30–200 Hz)优先使动作电位输出orexinLH细胞沉默。相反,低频(δ-θ,≈0.5-7Hz)类似地允许来自不同LH电池类型的输出。通过振荡频率对食欲素和非毒素细胞的这种差异控制是由细胞特异性,与阻抗无关的共振机制介导的。这些结果证实了电振荡作为LH放电的细胞类型特异性控制的一种新颖的输入方式,它提供了一种无法预料的方式来控制这种高度异质的神经元簇内的特定细胞集合。

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