Long noncoding RNA small nucleolar RNA host gene 5 facilitates neuropathic pain in spinal nerve injury by promoting SCN9A expression via CDK9

IF 4.3 3区 生物学
Changsheng Wang, Rongsheng Chen, Xitian Zhu, Xiaobo Zhang, Nancheng Lian
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Abstract

This study aims to explore the functions and mechanisms of long noncoding RNA small nucleolar RNA host gene 5 (SNHG5) in chronic constriction injury (CCI)-induced neuropathic pain (NP). An NP rat model was established using the CCI method and the NP severity was evaluated by paw withdrawal threshold (PWT) and paw withdrawal latency (PWL). The expression of SNHG5, CDK9, and SCN9A was quantified in rat dorsal root ganglion, in addition to the detections of apoptosis, pathological changes, neuron number, and the co-localization of Nav1.7 and cleaved caspase-3 with NeuN. In ND7/23 cells, the apoptosis and lactate dehydrogenase concentration were assessed, as well as the relationship between SNHG5, CDK9, and SCN9A. In the dorsal root ganglion of CCI-treated rats, SNHG5 and SCN9A were upregulated and downregulation of SNHG5 suppressed SCN9A expression, increased the PWT and PWL, blocked neuroinflammation and neuronal apoptosis, and alleviated NP. Mechanistically, SNHG5 recruited CDK9 to enhance SCN9A-encoded Nav1.7 expression and promoted peripheral neuronal apoptosis and injury. In addition, SCN9A overexpression nullified the alleviative effects of SNHG5 deficiency on NP and neuron loss in CCI rats. In conclusion, SNHG5 promotes SCN9A-encoded Nav1.7 expression by recruiting CDK9, thereby facilitating neuron loss and NP after spinal nerve injury, which may offer a promising target for the management of NP.

Abstract Image

长非编码 RNA 小核 RNA 宿主基因 5 通过 CDK9 促进 SCN9A 的表达,从而促进脊神经损伤中的神经病理性疼痛
本研究旨在探讨长非编码RNA小核仁RNA宿主基因5(SNHG5)在慢性收缩性损伤(CCI)诱导的神经病理性疼痛(NP)中的功能和机制。采用CCI方法建立了NP大鼠模型,并通过爪退缩阈值(PWT)和爪退缩潜伏期(PWL)评估了NP的严重程度。除了检测神经元凋亡、病理变化、神经元数量以及Nav1.7和裂解的caspase-3与NeuN共定位外,还量化了大鼠背根神经节中SNHG5、CDK9和SCN9A的表达。在 ND7/23 细胞中,评估了细胞凋亡和乳酸脱氢酶浓度,以及 SNHG5、CDK9 和 SCN9A 之间的关系。在CCI处理的大鼠背根神经节中,SNHG5和SCN9A上调,下调SNHG5可抑制SCN9A的表达,增加PWT和PWL,阻止神经炎症和神经元凋亡,缓解NP。从机制上讲,SNHG5 招募 CDK9 以增强 SCN9A 编码的 Nav1.7 的表达,并促进外周神经元凋亡和损伤。此外,SCN9A 的过表达抵消了 SNHG5 缺乏对 CCI 大鼠 NP 和神经元缺失的缓解作用。总之,SNHG5通过招募CDK9促进SCN9A编码的Nav1.7的表达,从而促进脊神经损伤后的神经元丢失和NP,这可能为NP的治疗提供了一个有前景的靶点。
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来源期刊
Human Cell
Human Cell 生物-细胞生物学
CiteScore
6.60
自引率
2.30%
发文量
176
期刊介绍: Human Cell is the official English-language journal of the Japan Human Cell Society. The journal serves as a forum for international research on all aspects of the human cell, encompassing not only cell biology but also pathology, cytology, and oncology, including clinical oncology. Embryonic stem cells derived from animals, regenerative medicine using animal cells, and experimental animal models with implications for human diseases are covered as well. Submissions in any of the following categories will be considered: Research Articles, Cell Lines, Rapid Communications, Reviews, and Letters to the Editor. A brief clinical case report focusing on cellular responses to pathological insults in human studies may also be submitted as a Letter to the Editor in a concise and short format. Not only basic scientists but also gynecologists, oncologists, and other clinical scientists are welcome to submit work expressing new ideas or research using human cells.
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