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Sensory Neuron Diversity in the Inner Ear Is Shaped by Activity

机译:内耳的感觉神经元多样性由活动塑造

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In the auditory system, type I spiral ganglion neurons (SGNs) convey complex acoustic information from inner hair cells (IHCs) to the brainstem. Although SGNs exhibit variation in physiological and anatomical properties, it is unclear which features are endogenous and which reflect input from synaptic partners. Using single-cell RNA sequencing, we derived a molecular classification of mouse type I SGNs comprising three subtypes that express unique combinations of Ca2+ binding proteins, ion channel regulators, guidance molecules, and transcription factors. Based on connectivity and susceptibility to age-related loss, these subtypes correspond to those defined physiologically. Additional intrinsic differences among subtypes and across the tonotopic axis highlight an unexpectedly active role for SGNs in auditory processing. SGN identities emerge postnatally and are disrupted in a mouse model of deafness that lacks IHC-driven activity. These results elucidate the range, nature, and origins of SGN diversity, with implications for treatment of congenital deafness.
机译:在听觉系统中,I型螺旋神经节神经元(SGNS)从内毛细胞(IHC)传达到脑干的复杂声学信息。虽然SGNS表现出生理和解剖学性质的变化,但目前尚不清楚哪种特征是内源性的,其反映了突触伴侣的输入。使用单细胞RNA测序,我们衍生出小鼠型I SGN的分子分类,其包含三种亚型,其表达Ca2 +结合蛋白,离子通道调节剂,引导分子和转录因子的独特组合。基于与年龄相关损失的连通性和易感性,这些亚型对应于生理学上定义的那些。亚型和跨音透镜轴之间的额外内在差异突出了检测处理中SGN的出乎意料的积极作用。 SGN标识出现后出现,并且在缺乏IHC驱动的活动的耳聋模型中被破坏。这些结果阐明了SGN多样性的范围,性质和起源,具有治疗先天性耳聋的影响。

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