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在幼虫中,POU 结构域蛋白 Pdm3 控制内部感觉神经元轴突投射模式的多样性。

Diversity of Internal Sensory Neuron Axon Projection Patterns Is Controlled by the POU-Domain Protein Pdm3 in Larvae.

机构信息

Department of Neuroscience, Columbia University, New York, New York 10027,

Department of Physiology and Cellular Biophysics, Columbia University Medical Center, New York, New York 10032, and.

出版信息

J Neurosci. 2018 Feb 21;38(8):2081-2093. doi: 10.1523/JNEUROSCI.2125-17.2018. Epub 2018 Jan 24.

Abstract

Internal sensory neurons innervate body organs and provide information about internal state to the CNS to maintain physiological homeostasis. Despite their conservation across species, the anatomy, circuitry, and development of internal sensory systems are still relatively poorly understood. A largely unstudied population of larval sensory neurons, termed tracheal dendrite (td) neurons, innervate internal respiratory organs and may serve as a model for understanding the sensing of internal states. Here, we characterize the peripheral anatomy, central axon projection, and diversity of td sensory neurons. We provide evidence for prominent expression of specific gustatory receptor genes in distinct populations of td neurons, suggesting novel chemosensory functions. We identify two anatomically distinct classes of td neurons. The axons of one class project to the subesophageal zone (SEZ) in the brain, whereas the other terminates in the ventral nerve cord (VNC). We identify expression and a developmental role of the POU-homeodomain transcription factor Pdm3 in regulating the axon extension and terminal targeting of SEZ-projecting td neurons. Remarkably, ectopic Pdm3 expression is alone sufficient to switch VNC-targeting axons to SEZ targets, and to induce the formation of putative synapses in these ectopic target zones. Our data thus define distinct classes of td neurons, and identify a molecular factor that contributes to diversification of axon targeting. These results introduce a tractable model to elucidate molecular and circuit mechanisms underlying sensory processing of internal body status and physiological homeostasis. How interoceptive sensory circuits develop, including how sensory neurons diversify and target distinct central regions, is still poorly understood, despite the importance of these sensory systems for maintaining physiological homeostasis. Here, we characterize classes of internal sensory neurons (td neurons) and uncover diverse axonal projections and expression of chemosensory receptor genes. We categorize td neurons into two classes based on dichotomous axon target regions, and identify the expression and role of the transcription factor Pdm3 in mediating td axon targeting to one of these target regions. Our results provide an entry point into studying internal sensory circuit development and function, and establish Pdm3 as a regulator of interoceptive axon targeting.

摘要

内部感觉神经元支配着身体器官,并向中枢神经系统提供有关内部状态的信息,以维持生理稳态。尽管它们在物种间具有保守性,但内部感觉系统的解剖结构、回路和发育仍然相对了解较少。一个在很大程度上尚未被研究的幼虫感觉神经元群体,称为气管树突(td)神经元,支配着内部呼吸器官,可能是理解内部状态感知的模型。在这里,我们描述了 td 感觉神经元的外周解剖结构、中枢轴突投射和多样性。我们提供了证据表明,特定的味觉受体基因在 td 神经元的特定群体中表达明显,这表明了新的化学感觉功能。我们确定了两种解剖上不同的 td 神经元类群。一类神经元的轴突投射到脑的食管下区(SEZ),而另一类则终止于腹神经索(VNC)。我们鉴定了两个在解剖上不同的 td 神经元类群。一类神经元的轴突投射到脑的食管下区(SEZ),而另一类则终止于腹神经索(VNC)。我们鉴定了 POU 同源域转录因子 Pdm3 的表达和发育作用,该因子调节 SEZ 投射 td 神经元的轴突延伸和末端靶向。值得注意的是,异位 Pdm3 表达本身就足以将靶向 VNC 的轴突切换到 SEZ 靶点,并在这些异位靶点区域诱导形成假定的突触。我们的数据因此定义了不同类别的 td 神经元,并确定了一个分子因子,该因子有助于轴突靶向的多样化。这些结果引入了一个可处理的模型,以阐明内部身体状态和生理稳态的感觉处理的分子和电路机制。尽管这些感觉系统对维持生理稳态很重要,但内部感觉回路如何发育,包括感觉神经元如何多样化并靶向不同的中枢区域,仍然知之甚少。在这里,我们描述了内部感觉神经元(td 神经元)的类别,并发现了不同的轴突投射和化学感觉受体基因的表达。我们根据二分叉轴突靶区将 td 神经元分为两类,并鉴定了转录因子 Pdm3 在介导 td 轴突靶向到其中一个靶区中的表达和作用。我们的结果为研究内部感觉回路的发育和功能提供了一个切入点,并确立了 Pdm3 作为内部感觉轴突靶向的调节剂。

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