Gonçalves Raquel M, Saggese Taryn, Yong Zhiyao, Ferreira Joana R, Ignatius Anita, Wilke Hans-Joachim, Neidlinger-Wilke Cornelia, Teixeira Graciosa Q
Institute of Orthopaedic Research and Biomechanics, Trauma Research Centre, Ulm University, Ulm, Germany.
Instituto de Investigação e Inovação Em Saúde (i3S), Universidade Do Porto, Porto, Portugal.
Front Bioeng Biotechnol. 2022 Jan 28;9:802789. doi: 10.3389/fbioe.2021.802789. eCollection 2021.
Mesenchymal stem/stromal cell (MSC)-based therapies for low back pain and intervertebral disc (IVD) degeneration have been emerging, despite the poor knowledge of their full mechanism of action. As failure of the annulus fibrosus (AF) is often associated with IVD herniation and inflammation, the objective of the present study was to investigate the impact of the MSC secretome on human AF cells exposed to mechanical loading and a pro-inflammatory environment. Human AF cells isolated from IVD biopsies from patients with adolescent idiopathic scoliosis (AIS) or disc degeneration (DD) were exposed to physiological cyclic tensile strain (CTS) for 72 h in a custom-made device, with or without interleukin (IL)-1β medium supplementation. AF cells stimulated with CTS + IL-1β were then treated with secretome from IL-1β-preconditioned MSCs for 48 h. AF cell metabolic activity, gene expression, protein secretion, matrix metalloproteinase (MMP) activity, and tissue inhibitor of MMPs (TIMP) concentration were evaluated. Expanded AF cells from AIS and DD patients revealed similar metabolic activity and gene expression profiles. CTS stimulation upregulated collagen type I () expression, while IL-1β significantly stimulated , , , and gene expression and prostaglandin E production by AF cells but downregulated . The combination of CTS + IL-1β had a similar outcome as IL-1β alone, accompanied by a significant upregulation of elastin. The MSC secretome did not show any immunomodulatory effect on CTS + IL-1β-stimulated AF cells but significantly decreased , MMP-2, , and , while increasing the production of TIMP-1. The obtained results demonstrate a stronger impact of the inflammatory milieu on human AF cells than upper physiologic mechanical stress. In addition, a new MSC mechanism of action in degenerated IVD consisting of the modulation of AF MMP activity was also evidenced, contributing to the advancement of knowledge in AF tissue metabolism.
尽管对基于间充质干/基质细胞(MSC)治疗腰痛和椎间盘(IVD)退变的完整作用机制了解甚少,但相关疗法已不断涌现。由于纤维环(AF)功能障碍常与IVD突出和炎症相关,本研究旨在探讨MSC分泌组对暴露于机械负荷和促炎环境的人AF细胞的影响。从青少年特发性脊柱侧凸(AIS)或椎间盘退变(DD)患者的IVD活检中分离出的人AF细胞,在定制装置中暴露于生理循环拉伸应变(CTS)72小时,添加或不添加白细胞介素(IL)-1β培养基。然后用来自IL-1β预处理的MSC的分泌组处理经CTS + IL-1β刺激的AF细胞48小时。评估AF细胞的代谢活性、基因表达、蛋白质分泌、基质金属蛋白酶(MMP)活性和MMP组织抑制剂(TIMP)浓度。来自AIS和DD患者的扩增AF细胞显示出相似的代谢活性和基因表达谱。CTS刺激上调I型胶原()表达,而IL-1β显著刺激AF细胞的、、和基因表达以及前列腺素E的产生,但下调。CTS + IL-1β的组合与单独使用IL-1β有相似的结果,同时弹性蛋白显著上调。MSC分泌组对CTS + IL-1β刺激的AF细胞未显示任何免疫调节作用,但显著降低了、MMP-2、和,同时增加了TIMP-1的产生。所得结果表明,炎症环境对人AF细胞的影响比生理上的机械应力更大。此外,还证实了MSC在退变IVD中的一种新的作用机制,即调节AF的MMP活性,这有助于增进对AF组织代谢的认识。
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