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嘌呤能受体 P2rx3 是发育过程中螺旋神经节神经元分支细化所必需的。

The Purinergic Receptor P2rx3 is Required for Spiral Ganglion Neuron Branch Refinement during Development.

机构信息

Department of Biology, Georgetown University, Washington, DC 20007.

Department of Biology, Georgetown University, Washington, DC 20007

出版信息

eNeuro. 2020 Aug 10;7(4). doi: 10.1523/ENEURO.0179-20.2020. Print 2020 Jul/Aug.

Abstract

The mammalian cochlea undergoes a highly dynamic process of growth and innervation during development. This process includes spiral ganglion neuron (SGN) branch refinement, a process whereby Type I SGNs undergo a phase of "debranching" before forming unramified synaptic contacts with inner hair cells. Using and as a strategy to genetically label individual SGNs in mice of both sexes, we report on both a time course of SGN branch refinement and a role for P2rx3 in this process. P2rx3 is an ionotropic ATP receptor that was recently implicated in outer hair cell spontaneous activity and Type II SGN synapse development (Ceriani et al., 2019), but its function in Type I SGN development is unknown. Here, we demonstrate that P2rx3 is expressed by Type I SGNs and hair cells during developmental periods that coincide with SGN branching refinement. null mice show SGNs with more complex branching patterns on their peripheral synaptic terminals and near their cell bodies around the time of birth. Loss of does not appear to confer general changes in axon outgrowth or hair cell formation, and alterations in branching complexity appear to mostly recover by postnatal day (P)6. However, when we examined the distribution of Type I SGN subtypes using antibodies that bind Calb2, Calb1, and Pou4f1, we found that null mice showed an increased proportion of SGNs that express Calb2. These data suggest P2rx3 may be necessary for normal Type I SGN differentiation in addition to serving a role in branch refinement.

摘要

哺乳动物耳蜗在发育过程中经历高度动态的生长和神经支配过程。这个过程包括螺旋神经节神经元(SGN)的分支细化,其中 I 型 SGN 经历一个“去分支”的阶段,然后才与内毛细胞形成无分支的突触接触。我们使用 和 作为在雌雄小鼠中分别标记单个 SGN 的策略,报告了 SGN 分支细化的时间进程以及 P2rx3 在这个过程中的作用。P2rx3 是一种离子型 ATP 受体,最近被牵连到外毛细胞自发性活动和 II 型 SGN 突触发育中(Ceriani 等人,2019),但其在 I 型 SGN 发育中的功能尚不清楚。在这里,我们证明 P2rx3 在与 SGN 分支细化同时发生的发育时期由 I 型 SGN 和毛细胞表达。在出生前后, P2rx3 缺失小鼠的外周突触末梢和细胞体附近的 SGN 具有更复杂的分支模式。缺失似乎不会导致轴突生长或毛细胞形成的普遍变化,并且分支复杂性的改变似乎主要在出生后第 6 天(P6)恢复。然而,当我们使用结合 Calb2、Calb1 和 Pou4f1 的抗体来检查 I 型 SGN 亚型的分布时,我们发现 P2rx3 缺失小鼠表达 Calb2 的 SGN 比例增加。这些数据表明,P2rx3 可能除了在分支细化中起作用外,对于正常的 I 型 SGN 分化也是必要的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0cf4/7418533/b23e0cd6d231/SN-ENUJ200185F001.jpg

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