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多样性很重要——通过内毛细胞的异质突触扩展声音强度编码。

Diversity matters - extending sound intensity coding by inner hair cells via heterogeneous synapses.

机构信息

Institute for Auditory Neuroscience and InnerEarLab, University Medical Center Göttingen, Göttingen, Germany.

Auditory Neuroscience and Synaptic Nanophysiology Group, Max Planck Institute for Multidisciplinary Sciences, Göttingen, Germany.

出版信息

EMBO J. 2023 Dec 1;42(23):e114587. doi: 10.15252/embj.2023114587. Epub 2023 Oct 6.

Abstract

Our sense of hearing enables the processing of stimuli that differ in sound pressure by more than six orders of magnitude. How to process a wide range of stimulus intensities with temporal precision is an enigmatic phenomenon of the auditory system. Downstream of dynamic range compression by active cochlear micromechanics, the inner hair cells (IHCs) cover the full intensity range of sound input. Yet, the firing rate in each of their postsynaptic spiral ganglion neurons (SGNs) encodes only a fraction of it. As a population, spiral ganglion neurons with their respective individual coding fractions cover the entire audible range. How such "dynamic range fractionation" arises is a topic of current research and the focus of this review. Here, we discuss mechanisms for generating the diverse functional properties of SGNs and formulate testable hypotheses. We postulate that an interplay of synaptic heterogeneity, molecularly distinct subtypes of SGNs, and efferent modulation serves the neural decomposition of sound information and thus contributes to a population code for sound intensity.

摘要

我们的听觉能够处理声音压力差异超过六个数量级的刺激。如何以时间精度处理广泛的刺激强度是听觉系统一个神秘的现象。在主动耳蜗微力学的动态范围压缩之后,内毛细胞 (IHC) 覆盖了声音输入的全强度范围。然而,每个突触后的螺旋神经节神经元 (SGN) 的发放率只编码了其中的一部分。作为一个群体,具有各自编码分数的螺旋神经节神经元覆盖了整个可听范围。这种“动态范围分馏”是如何产生的,是当前研究的一个课题,也是本综述的重点。在这里,我们讨论了产生 SGN 多样化功能特性的机制,并提出了可测试的假设。我们假设,突触异质性、分子上不同的 SGN 亚型和传出调制的相互作用为声音信息的神经分解提供了服务,从而为声音强度的群体编码做出了贡献。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6f2d/10690447/c09391870b00/EMBJ-42-e114587-g009.jpg

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