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全基因组分析确定慢性重叠疼痛病症中轴突发生受损。

Genome-wide analysis identifies impaired axonogenesis in chronic overlapping pain conditions.

作者信息

Khoury Samar, Parisien Marc, Thompson Scott J, Vachon-Presseau Etienne, Roy Mathieu, Martinsen Amy E, Winsvold Bendik S, Mundal Ingunn P, Zwart John-Anker, Kania Artur, Mogil Jeffrey S, Diatchenko Luda

机构信息

Alan Edwards Centre for Research on Pain, McGill University, Montreal, QC H3A 0G1, Canada.

Faculty of Dental Medicine and Oral Health Sciences, McGill University, Montreal, QC H3A 0G1, Canada.

出版信息

Brain. 2022 Apr 29;145(3):1111-1123. doi: 10.1093/brain/awab359.

Abstract

Chronic pain is often present at more than one anatomical location, leading to chronic overlapping pain conditions. Whether chronic overlapping pain conditions represent a distinct pathophysiology from the occurrence of pain at only one site is unknown. Using genome-wide approaches, we compared genetic determinants of chronic single-site versus multisite pain in the UK Biobank. We found that different genetic signals underlie chronic single-site and multisite pain with much stronger genetic contributions for the latter. Among 23 loci associated with multisite pain, nine loci replicated in the HUNT cohort, with the DCC netrin 1 receptor (DCC) as the top gene. Functional genomics identified axonogenesis in brain tissues as the major contributing pathway to chronic multisite pain. Finally, multimodal structural brain imaging analysis showed that DCC is most strongly expressed in subcortical limbic regions and is associated with alterations in the uncinate fasciculus microstructure, suggesting that DCC-dependent axonogenesis may contribute to chronic overlapping pain conditions via corticolimbic circuits.

摘要

慢性疼痛通常存在于多个解剖位置,导致慢性重叠性疼痛病症。慢性重叠性疼痛病症是否代表一种与仅在一个部位发生疼痛截然不同的病理生理学尚不清楚。我们利用全基因组方法,在英国生物银行中比较了慢性单部位疼痛与多部位疼痛的遗传决定因素。我们发现,慢性单部位疼痛和多部位疼痛有着不同的遗传信号,后者的遗传贡献更强。在与多部位疼痛相关的23个基因座中,有9个基因座在HUNT队列中得到了验证,其中DCC神经纤毛蛋白1受体(DCC)是最重要的基因。功能基因组学确定脑组织中的轴突形成是导致慢性多部位疼痛的主要途径。最后,多模态脑结构成像分析表明,DCC在皮质下边缘区域表达最为强烈,并且与钩状束微结构的改变有关,这表明依赖DCC的轴突形成可能通过皮质边缘回路导致慢性重叠性疼痛病症。

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