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引用本文的文献

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胰岛素信号突变体的成年单细胞核神经元转录组揭示行为和学习的调节因子。

Adult Single-nucleus Neuronal Transcriptomes of Insulin Signaling Mutants Reveal Regulators of Behavior and Learning.

作者信息

Ange Jonathan St, Weng Yifei, Stevenson Morgan E, Kaletsky Rachel, Moore Rebecca S, Zhou Shiyi, Murphy Coleen T

出版信息

bioRxiv. 2024 Feb 7:2024.02.07.579364. doi: 10.1101/2024.02.07.579364.

DOI:10.1101/2024.02.07.579364
PMID:38370779
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10871314/
Abstract

UNLABELLED

The insulin/insulin-like signaling (IIS) pathway regulates many of adult functions, including learning and memory . While whole-worm and tissue-specific transcriptomic analyses have identified IIS targets , a higher-resolution single-cell approach is required to identify changes that confer neuron-specific improvements in the long-lived insulin receptor mutant, . To understand how behaviors that are controlled by a small number of neurons change in mutants, we used the deep resolution of single-nucleus RNA sequencing to define each neuron type's transcriptome in adult wild-type and mutants. First, we found surprising differences between wild-type L4 larval neurons and young adult neurons in chemoreceptor expression, synaptic genes, and learning and memory genes. These Day 1 adult neuron transcriptomes allowed us to identify adult AWC-specific regulators of chemosensory function and to predict neuron-to-neuron peptide/receptor pairs. We then identified gene expression changes that correlate with improved cognitive functions, particularly in the AWC sensory neuron that controls learning and associative memory , and used behavioral assays to test their roles in cognitive function. Combining deep single-neuron transcriptomics, genetic manipulation, and behavioral analyses enabled us to identify genes that may function in a single adult neuron to control behavior, including conserved genes that function in learning and memory.

ONE-SENTENCE SUMMARY: Single-nucleus sequencing of adult wild-type and neurons reveals functionally relevant transcriptional changes, including regulators of chemosensation, learning, and memory.

摘要

未标记

胰岛素/胰岛素样信号(IIS)通路调节许多成年功能,包括学习和记忆。虽然全虫和组织特异性转录组分析已经确定了IIS靶点,但需要更高分辨率的单细胞方法来识别在长寿胰岛素受体突变体中赋予神经元特异性改善的变化。为了了解由少数神经元控制的行为在突变体中如何变化,我们使用单核RNA测序的深度分辨率来定义成年野生型和突变体中每种神经元类型的转录组。首先,我们发现野生型L4幼虫神经元和年轻成年神经元在化学感受器表达、突触基因以及学习和记忆基因方面存在惊人差异。这些成年第1天神经元转录组使我们能够识别化学感觉功能的成年AWC特异性调节因子,并预测神经元间的肽/受体对。然后,我们确定了与改善的认知功能相关的基因表达变化,特别是在控制学习和联想记忆的AWC感觉神经元中,并使用行为分析来测试它们在认知功能中的作用。结合深度单神经元转录组学、基因操作和行为分析,使我们能够识别可能在单个成年神经元中发挥作用以控制行为的基因,包括在学习和记忆中起作用的保守基因。

一句话总结

成年野生型和突变体神经元的单核测序揭示了功能相关的转录变化,包括化学感觉、学习和记忆的调节因子。