Alpha-2 nicotinic acetylcholine receptors regulate spectral integration in auditory cortex.

IF 3.4 3区 医学 Q2 NEUROSCIENCES Frontiers in Neural Circuits Pub Date : 2024-11-01 eCollection Date: 2024-01-01 DOI:10.3389/fncir.2024.1492452
Irakli Intskirveli, Susan Gil, Ronit Lazar, Raju Metherate
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Abstract

Introduction: In primary auditory cortex (A1), nicotinic acetylcholine receptors (nAChRs) containing α2 subunits are expressed in layer 5 Martinotti cells (MCs)-inhibitory interneurons that send a main axon to superficial layers to inhibit distal apical dendrites of pyramidal cells (PCs). MCs also contact interneurons in supragranular layers that, in turn, inhibit PCs. Thus, MCs may regulate PCs via inhibition and disinhibition, respectively, of distal and proximal apical dendrites. Auditory inputs to PCs include thalamocortical inputs to middle layers relaying information about characteristic frequency (CF) and near-CF stimuli, and intracortical long-distance ("horizontal") projections to multiple layers carrying information about spectrally distant ("nonCF") stimuli. CF and nonCF inputs integrate to create broad frequency receptive fields (RFs). Systemic administration of nicotine activates nAChRs to "sharpen" RFs-to increase gain within a narrowed RF-resulting in enhanced responses to CF stimuli and reduced responses to nonCF stimuli. While nicotinic mechanisms to increase gain have been identified, the mechanism underlying RF narrowing is unknown.

Methods: Here, we examine the role of α2 nAChRs in mice with α2 nAChR-expressing neurons labeled fluorescently, and in mice with α2 nAChRs genetically deleted.

Results: The distribution of fluorescent neurons in auditory cortex was consistent with previous studies demonstrating α2 nAChRs in layer 5 MCs, including nonpyramidal somata in layer 5 and dense processes in layer 1. We also observed label in subcortical auditory regions, including processes, but no somata, in the medial geniculate body, and both fibers and somata in the inferior colliculus. Using electrophysiological (current-source density) recordings in α2 nAChR knock-out mice, we found that systemic nicotine failed to enhance CF-evoked inputs to layer 4, suggesting a role for subcortical α2 nAChRs, and failed to reduce nonCF-evoked responses, suggesting that α2 nAChRs regulate horizontal projections to produce RF narrowing.

Discussion: The results support the hypothesis that α2 nAChRs function to simultaneously enhance RF gain and narrow RF breadth in A1. Notably, a similar neural circuit may recur throughout cortex and hippocampus, suggesting widespread conserved functions regulated by α2 nAChRs.

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α-2烟碱乙酰胆碱受体调节听觉皮层的频谱整合。
简介:在初级听觉皮层(A1)中,含有α2亚单位的烟碱乙酰胆碱受体(nAChRs)表达于第5层的马蒂诺蒂细胞(Martinotti cells,MCs)--抑制性中间神经元,MCs将主轴突发送到浅层,以抑制锥体细胞(PCs)的远端顶端树突。MCs 还与上釉层的中间神经元联系,而上釉层的中间神经元反过来又抑制 PCs。因此,MC 可分别通过抑制和解除抑制远端和近端顶端树突来调节 PC。PC的听觉输入包括丘脑皮层输入到中层的特征频率(CF)和近CF刺激信息,以及皮层内长距离("水平")投射到多层的光谱遥远("非CF")刺激信息。CF和非CF输入整合成宽频感受野(RF)。全身注射尼古丁可激活 nAChRs,使射频 "锐化"--在缩小的射频范围内增加增益--从而增强对 CF 刺激的反应,降低对非 CF 刺激的反应。方法:我们在荧光标记了α2 nAChR表达神经元的小鼠和基因上删除了α2 nAChR的小鼠中研究了α2 nAChR的作用:听皮层中荧光神经元的分布与之前的研究一致,表明第 5 层 MC 中存在 α2 nAChRs,包括第 5 层的非锥体体细胞和第 1 层的致密过程。我们还在皮层下听觉区域观察到了标记,包括内侧膝状体的过程,但没有体节,以及下丘的纤维和体节。通过对α2 nAChR基因敲除小鼠的电生理(电流源密度)记录,我们发现全身性尼古丁不能增强第4层的CF诱发输入,这表明皮层下的α2 nAChRs起了作用,并且不能减少非CF诱发反应,这表明α2 nAChRs调节水平投射以产生RF缩小:讨论:研究结果支持α2 nAChRs在A1中同时增强射频增益和缩小射频宽度的假设。值得注意的是,类似的神经回路可能在整个大脑皮层和海马中反复出现,这表明α2 nAChRs调节的功能是广泛保守的。
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来源期刊
CiteScore
6.00
自引率
5.70%
发文量
135
审稿时长
4-8 weeks
期刊介绍: Frontiers in Neural Circuits publishes rigorously peer-reviewed research on the emergent properties of neural circuits - the elementary modules of the brain. Specialty Chief Editors Takao K. Hensch and Edward Ruthazer at Harvard University and McGill University respectively, are supported by an outstanding Editorial Board of international experts. This multidisciplinary open-access journal is at the forefront of disseminating and communicating scientific knowledge and impactful discoveries to researchers, academics and the public worldwide. Frontiers in Neural Circuits launched in 2011 with great success and remains a "central watering hole" for research in neural circuits, serving the community worldwide to share data, ideas and inspiration. Articles revealing the anatomy, physiology, development or function of any neural circuitry in any species (from sponges to humans) are welcome. Our common thread seeks the computational strategies used by different circuits to link their structure with function (perceptual, motor, or internal), the general rules by which they operate, and how their particular designs lead to the emergence of complex properties and behaviors. Submissions focused on synaptic, cellular and connectivity principles in neural microcircuits using multidisciplinary approaches, especially newer molecular, developmental and genetic tools, are encouraged. Studies with an evolutionary perspective to better understand how circuit design and capabilities evolved to produce progressively more complex properties and behaviors are especially welcome. The journal is further interested in research revealing how plasticity shapes the structural and functional architecture of neural circuits.
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