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Ptf1a的缺失导致脑干中广泛的细胞命运错误指定,影响躯体感觉和内脏感觉核的发育。

Loss of Ptf1a Leads to a Widespread Cell-Fate Misspecification in the Brainstem, Affecting the Development of Somatosensory and Viscerosensory Nuclei.

作者信息

Iskusnykh Igor Y, Steshina Ekaterina Y, Chizhikov Victor V

机构信息

Department of Anatomy and Neurobiology and.

Department of Anatomy and Neurobiology and The Neuroscience Institute, University of Tennessee Health Science Center, Memphis, Tennessee 38163

出版信息

J Neurosci. 2016 Mar 2;36(9):2691-710. doi: 10.1523/JNEUROSCI.2526-15.2016.

Abstract

UNLABELLED

The brainstem contains diverse neuronal populations that regulate a wide range of processes vital to the organism. Proper cell-fate specification decisions are critical to achieve neuronal diversity in the CNS, but the mechanisms regulating cell-fate specification in the developing brainstem are poorly understood. Previously, it has been shown that basic helix-loop-helix transcription factor Ptf1a is required for the differentiation and survival of neurons of the inferior olivary and cochlear brainstem nuclei, which contribute to motor coordination and sound processing, respectively. In this study, we show that the loss of Ptf1a compromises the development of the nucleus of the solitary tract, which processes viscerosensory information, and the spinal and principal trigeminal nuclei, which integrate somatosensory information of the face. Combining genetic fate-mapping, birth-dating, and gene expression studies, we found that at least a subset of brainstem abnormalities in Ptf1a(-/-) mice are mediated by a dramatic cell-fate misspecification in rhombomeres 2-7, which results in the production of supernumerary viscerosensory and somatosensory neurons of the Lmx1b lineage at the expense of Pax2(+) GABAergic viscerosensory and somatosensory neurons, and inferior olivary neurons. Our data identify Ptf1a as a major regulator of cell-fate specification decisions in the developing brainstem, and as a previously unrecognized developmental regulator of both viscerosensory and somatosensory brainstem nuclei.

SIGNIFICANCE STATEMENT

Cell-fate specification decisions are critical for normal CNS development. Although extensively studied in the cerebellum and spinal cord, the mechanisms mediating cell-fate decisions in the brainstem, which regulates a wide range of processes vital to the organism, remain largely unknown. Here we identified mouse Ptf1a as a novel regulator of cell-fate decisions during both early and late brainstem neurogenesis, which are critical for proper development of several major classes of brainstem cells, including neurons of the somatosensory and viscerosensory nuclei. Since loss-of-function PTF1A mutations were described in human patients, we suggest Ptf1a-dependent cell-fate misspecification as a novel mechanism of human brainstem pathology.

摘要

未标记

脑干包含多种神经元群体,它们调节着对机体至关重要的广泛生理过程。正确的细胞命运决定对于在中枢神经系统中实现神经元多样性至关重要,但发育中的脑干中调节细胞命运决定的机制却知之甚少。此前研究表明,碱性螺旋-环-螺旋转录因子Ptf1a是下橄榄核和耳蜗脑干核神经元分化和存活所必需的,这两个核分别参与运动协调和声音处理。在本研究中,我们发现Ptf1a的缺失会损害孤束核的发育,孤束核处理内脏感觉信息,以及脊髓和三叉神经主核的发育,这两个核整合面部的躯体感觉信息。结合遗传命运图谱、出生时间测定和基因表达研究,我们发现Ptf1a(-/-)小鼠脑干异常的至少一部分是由菱脑节2-7中显著的细胞命运错误指定介导的,这导致产生了额外的Lmx1b谱系的内脏感觉和躯体感觉神经元,代价是Pax2(+) GABA能内脏感觉和躯体感觉神经元以及下橄榄核神经元。我们的数据确定Ptf1a是发育中脑干细胞命运决定的主要调节因子,也是内脏感觉和躯体感觉脑干核以前未被认识到的发育调节因子。

意义声明

细胞命运决定对于中枢神经系统的正常发育至关重要。尽管在小脑和脊髓中进行了广泛研究,但介导脑干细胞命运决定的机制在很大程度上仍然未知,脑干调节着对机体至关重要的广泛生理过程。在这里,我们确定小鼠Ptf1a是脑干早期和晚期神经发生过程中细胞命运决定的新型调节因子,这对于包括躯体感觉和内脏感觉核神经元在内的几类主要脑干细胞的正常发育至关重要。由于在人类患者中描述了功能丧失的PTF1A突变,我们认为Ptf1a依赖性细胞命运错误指定是人类脑干病理学的一种新机制。

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