Osteocytes contribute to sex-specific differences in osteoarthritic pain.

IF 3.9 2区医学 Q2 ENDOCRINOLOGY & METABOLISM

Frontiers in Endocrinology Pub Date : 2024-11-07 eCollection Date: 2024-01-01 DOI:10.3389/fendo.2024.1480274

Ryan Jones, Sophie J Gilbert, Sarah R Christofides, Deborah J Mason

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Abstract

Osteoarthritic (OA) pain affects 18% of females and 9.6% of males aged over 60 worldwide, with 62% of all OA patients being women. The molecular drivers of sex-based differences in OA are unknown. Bone is intricately coupled with the sensory nervous system and one of the only joint tissues known to show changes that correlate with patient pain in OA. There are fundamental sex differences in pain sensation and bone biology which may be intrinsic to OA disease progression, however these differences are vastly under researched. We have utilised three data sets to investigate the hypothesis that potential mediators responsible for sex dependent pain mechanisms displayed in OA are derived from mechanically stimulated osteocytes. Our published dataset of the in vitro human osteocyte mechanosome was independently compared with published data from, sex-based gene expression differences in human long bone, the sex-based gene expression differences during the skeletal maturation of the mouse osteocyte transcriptome and sex specific OA risk factors and effector genes in a large human GWAS. 80 of the 377 sex-specific genes identified in the mouse osteocyte transcriptome were mechanically regulated in osteocytes with enrichment associated with neural crest migration and axon extension, and DISEASES analysis enrichment for the rheumatoid arthritis pathway. 3861 mechanically regulated osteocytic genes displayed sex-specific differences in human long bone with enrichment for genes associated with the synapse, sensory perception of pain, axon guidance, immune responses, distal peripheral sensory neuropathy, sensory neuropathy, and poor wound healing. 32 of 77 effector genes and 1 of 3 female specific OA risk factor genes identified in the human GWAS were differentially expressed in the osteocyte mechanosome and male and female bone. This analysis lends support to the hypothesis that mechanically regulated genes in osteocytes could influence sex specific differences in osteoarthritic pain and highlights pain pathways with approved drugs that could potentially treat elevated pain susceptibility in females with OA.

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骨细胞导致骨关节炎疼痛的性别差异。

全球 60 岁以上人群中，18% 的女性和 9.6% 的男性患有骨关节炎（OA）疼痛，其中 62% 的 OA 患者为女性。造成 OA 性别差异的分子驱动因素尚不清楚。骨骼与感觉神经系统密切相关，是已知唯一能显示与 OA 患者疼痛相关的变化的关节组织之一。痛觉和骨生物学方面存在着根本性的性别差异，这可能是导致 OA 疾病进展的内在因素，但对这些差异的研究还远远不够。我们利用三个数据集研究了一个假设，即造成 OA 中性别依赖性疼痛机制的潜在介质来自机械刺激的骨细胞。我们将已发表的体外人类骨细胞机械体数据集与已发表的以下数据进行了独立比较：人类长骨中基于性别的基因表达差异、小鼠骨细胞转录组骨骼成熟过程中基于性别的基因表达差异以及大型人类 GWAS 中的特定性别 OA 风险因素和效应基因。在小鼠成骨细胞转录组中发现的377个性别特异性基因中，有80个在成骨细胞中受到机械调控，其富集与神经嵴迁移和轴突延伸有关，而DISEASES分析则富集了类风湿性关节炎通路。在人类长骨中，3861 个受机械调控的骨细胞基因显示出性别特异性差异，与突触、痛觉感知、轴突导向、免疫反应、远端外周感觉神经病、感觉神经病和伤口愈合不良相关的基因富集。在人类 GWAS 中发现的 77 个效应基因中的 32 个基因和 3 个女性特异性 OA 风险因子基因中的 1 个基因在骨细胞机械体和男性与女性骨骼中的表达存在差异。这项分析支持这样的假设，即骨细胞中的机械调控基因可能影响骨关节炎疼痛的性别差异，并突出了已获批准药物的疼痛通路，这些药物有可能治疗女性 OA 患者的疼痛易感性升高。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Frontiers in Endocrinology Medicine-Endocrinology, Diabetes and Metabolism

CiteScore

5.70

自引率

9.60%

发文量

3023

审稿时长

14 weeks

期刊介绍： Frontiers in Endocrinology is a field journal of the "Frontiers in" journal series. In today’s world, endocrinology is becoming increasingly important as it underlies many of the challenges societies face - from obesity and diabetes to reproduction, population control and aging. Endocrinology covers a broad field from basic molecular and cellular communication through to clinical care and some of the most crucial public health issues. The journal, thus, welcomes outstanding contributions in any domain of endocrinology. Frontiers in Endocrinology publishes articles on the most outstanding discoveries across a wide research spectrum of Endocrinology. The mission of Frontiers in Endocrinology is to bring all relevant Endocrinology areas together on a single platform.