从 C1-2 节段切除手术中恢复的人体 C2 背根神经节的单细胞特征:对颈部疼痛的影响。

Asta Arendt-Tranholm, Ishwarya Sankaranarayanan, Cathryn Payne, Marisol Mancilla Moreno, Khadijah Mazhar, Natalie Yap, Abby P Chiu, Allison Barry, Pooja P Patel, Nikhil N Inturi, Diana Tavares Ferreira, Anubhav Amin, Mahesh Karandikar, Jeffrey G Jarvik, Judith A Turner, Christoph P Hofstetter, Michele Curatolo, Theodore J Price
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引用次数: 0

摘要

背根神经节(DRG)中的神经元接收和传递来自其支配的组织和外部环境的感觉信息。上颈(C1-C2) DRGs在功能上是独特的,因为它们接受来自颈部、头部和枕颅硬脑膜的输入,后两者也受三叉神经节(TG)的支配。C2 DRG在颈痛中也起着重要作用,颈痛是一种常见的致残性疾病,但人们对其了解甚少。先进的转录组学方法显著提高了我们在单细胞分辨率下表征DRG和TG中RNA表达模式的能力,但之前没有研究表征C2 DRG。我们的目的是使用单核和空间转录组学方法来创建关节置换术合并神经节切除术患者的C2 DRGs分子图谱。在之前的基因组和转录组全关联研究(GWAS/TWAS)中发现的急性(FGFBP2, C8orf34和EFNA1)患者。我们的工作建立了人类C2 DRG图谱,并确定了与慢性颈部疼痛相关的基因表达模式的改变。这项工作为探索人类影响颈椎的疼痛疾病奠定了基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Single-cell characterization of the human C2 dorsal root ganglion recovered from C1-2 arthrodesis surgery: implications for neck pain.

Neurons in the dorsal root ganglion (DRG) receive and transmit sensory information from the tissues they innervate and from the external environment. Upper cervical (C1-C2) DRGs are functionally unique as they receive input from the neck, head, and occipital cranial dura, the latter two of which are also innervated by the trigeminal ganglion (TG). The C2 DRG also plays an important role in neck pain, a common and disabling disorder that is poorly understood. Advanced transcriptomic approaches have significantly improved our ability to characterize RNA expression patterns at single-cell resolution in the DRG and TG, but no previous studies have characterized the C2 DRG. Our aim was to use single-nucleus and spatial transcriptomic approaches to create a molecular map of C2 DRGs from patients undergoing arthrodesis surgery with ganglionectomy. Patients with acute (<3 months) or chronic (≥3 months) neck pain were enrolled and completed patient-reported outcomes and quantitative sensory testing prior to surgery. C2 DRGs were characterized with bulk, single nucleus, and spatial RNA sequencing technologies from 22 patients. Through a comparative analysis to published datasets of the lumbar DRG and TG, neuronal clusters identified in both TG and DRG were identified in the C2 DRG. Therefore, our study definitively characterizes the molecular composition of human C2 neurons and establishes their similarity with unique characteristics of subsets of TG neurons. We identified differentially expressed genes in endothelial, fibroblast and myelinating Schwann cells associated with chronic pain, including FGFBP2, C8orf34 and EFNA1 which have been identified in previous genome and transcriptome wide association studies (GWAS/TWAS). Our work establishes an atlas of the human C2 DRG and identifies altered gene expression patterns associated with chronic neck pain. This work establishes a foundation for the exploration of painful disorders in humans affecting the cervical spine.

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