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树突非线性的非均匀分布差异地将丘脑纹状体和皮质纹状体输入作用于胆碱能中间神经元。

Non-uniform distribution of dendritic nonlinearities differentially engages thalamostriatal and corticostriatal inputs onto cholinergic interneurons.

机构信息

Department of Medical Neurobiology, Institute of Medical Research Israel - Canada, The Faculty of Medicine, Jerusalem, Israel.

Edmond and Lily Safra Center for Brain Sciences, The Hebrew University of Jerusalem, Jerusalem, Israel.

出版信息

Elife. 2022 Jul 11;11:e76039. doi: 10.7554/eLife.76039.

Abstract

The tonic activity of striatal cholinergic interneurons (CINs) is modified differentially by their afferent inputs. Although their unitary synaptic currents are identical, in most CINs cortical inputs onto distal dendrites only weakly entrain them, whereas proximal thalamic inputs trigger abrupt pauses in discharge in response to salient external stimuli. To test whether the dendritic expression of the active conductances that drive autonomous discharge contribute to the CINs' capacity to dissociate cortical from thalamic inputs, we used an optogenetics-based method to quantify dendritic excitability in mouse CINs. We found that the persistent sodium (NaP) current gave rise to dendritic boosting, and that the hyperpolarization-activated cyclic nucleotide-gated (HCN) current gave rise to a subhertz membrane resonance. This resonance may underlie our novel finding of an association between CIN pauses and internally-generated slow wave events in sleeping non-human primates. Moreover, our method indicated that dendritic NaP and HCN currents were preferentially expressed in proximal dendrites. We validated the non-uniform distribution of NaP currents: pharmacologically; with two-photon imaging of dendritic back-propagating action potentials; and by demonstrating boosting of thalamic, but not cortical, inputs by NaP currents. Thus, the localization of active dendritic conductances in CIN dendrites mirrors the spatial distribution of afferent terminals and may promote their differential responses to thalamic . cortical inputs.

摘要

纹状体胆碱能中间神经元(CINs)的紧张活动受到传入输入的不同调节。尽管它们的单位突触电流是相同的,但在大多数 CINs 中,皮质输入到远端树突仅微弱地使它们兴奋,而近端丘脑输入则会在外来刺激下引发突然的放电暂停。为了测试驱动自主放电的主动电导在 CINs 区分皮质和丘脑输入的能力中的表达情况,我们使用基于光遗传学的方法来定量小鼠 CINs 的树突兴奋性。我们发现持续钠 (NaP) 电流引起树突增强,而超极化激活环核苷酸门控 (HCN) 电流引起亚赫兹膜共振。这种共振可能是我们在非人类灵长类动物睡眠中发现 CIN 暂停与内部产生的慢波事件之间存在关联的基础。此外,我们的方法表明,树突 NaP 和 HCN 电流优先在近端树突中表达。我们验证了 NaP 电流的非均匀分布:通过药理学;通过双光子成像树突反向传播动作电位;并通过证明 NaP 电流增强了丘脑而不是皮质输入。因此,活性树突电导在 CIN 树突中的定位反映了传入终端的空间分布,并可能促进它们对丘脑的不同反应。. 皮质输入。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/44cd/9302969/4eeac0bedc79/elife-76039-fig1.jpg

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