转化生长因子-β通过p38和p44/42丝裂原活化蛋白激酶的部分激活诱导人黄韧带衍生细胞分泌白细胞介素-6。

IF 2.3 Q2 ORTHOPEDICS
Asian Spine Journal Pub Date : 2023-12-01 Epub Date: 2023-11-10 DOI:10.31616/asj.2023.0025
Yuta Goto, Kenji Kato, Kiyoshi Yagi, Yohei Kawaguchi, Hiroki Yonezu, Tomoko Koshimae, Yuko Waguri-Nagaya, Hideki Murakami, Nobuyuki Suzuki
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引用次数: 0

摘要

研究设计:本实验研究使用人黄韧带衍生细胞(HFCs)进行。目的:探讨转化生长因子-β(TGF-β)刺激的HFCs分泌白细胞介素-6(IL-6)的细胞内信号机制。文献综述:腰椎管狭窄症(LSS)是一种在老年人中流行的疾病,其特征是下肢疼痛。尽管近年来LSS患者的数量有所增加,但其潜在的病理机制仍不清楚。临床检查通常依靠磁共振成像来诊断患者,显示黄韧带肥大。一些研究表明,黄韧带肥大与炎症/纤维化之间存在关联,在手术获得的黄韧带样本中观察到TGF-β和IL-6的表达。然而,缺乏将TGF-β和IL-6在HFCs中表达联系起来的直接证据。方法:从接受减压手术的LSS患者中获得HFCs。用TGF-β刺激细胞,并用p38丝裂原活化蛋白(MAP)激酶抑制剂SB203580或p44/42 MAP激酶抑制剂FR180204预处理。分别使用酶联免疫测定和实时聚合酶链式反应分析细胞培养基中IL-6的分泌和IL-6信使RNA(mRNA)的表达水平。结果:TGF-β给药可引起IL-6释放的剂量和时间依赖性刺激。SB203580和FR180204治疗显著抑制TGF-β诱导的HFCs分泌IL-6。此外,这些抑制剂抑制了对TGF-β刺激的IL-6 mRNA表达。结论:TGF-β通过激活p38或p44/42 MAP激酶,诱导HFCs中IL-6蛋白分泌和基因表达。这些结果表明,IL-6介导的炎症反应与LSS的组织肥大之间存在潜在联系,我们通过使用HFCs分析MAP激酶途径,深入了解了针对LSS相关炎症的治疗干预的分子靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Transforming Growth Factor-β Induces Interleukin-6 Secretion from Human Ligamentum Flavum-Derived Cells through Partial Activation of p38 and p44/42 Mitogen-Activated Protein Kinases.

Study design: This experimental study was performed using human ligamentum flavum-derived cells (HFCs).

Purpose: To investigate the intracellular signaling mechanism of interleukin-6 (IL-6) secretion in transforming growth factor-β (TGF- β)-stimulated HFCs.

Overview of literature: Lumbar spinal stenosis (LSS) is a prevalent disease among the elderly, characterized by debilitating pain in the lower extremities. Although the number of patients with LSS has increased in recent years, the underlying pathomechanism remains unclear. Clinical examinations typically rely on magnetic resonance imaging to diagnose patients, revealing ligamentum flavum hypertrophy. Some studies have suggested an association between ligamentum flavum hypertrophy and inflammation/fibrosis, and expression of TGF-β and IL-6 has been observed in surgically obtained ligamentum flavum samples. However, direct evidence linking TGF-β and IL-6 expression in HFCs is lacking.

Methods: HFCs were obtained from patients with LSS who had undergone decompression surgery. The cells were stimulated with TGF-β and pretreated with either the p38 mitogen-activated protein (MAP) kinase inhibitor SB203580 or the p44/42 MAP kinase inhibitor FR180204. IL-6 secretion in the cell culture medium and IL-6 messenger RNA (mRNA) expression levels were analyzed using an enzyme-linked immunoassay and real-time polymerase chain reaction, respectively.

Results: TGF-β administration resulted in a dose- and time-dependent stimulation of IL-6 release. Treatment with SB203580 and FR180204 markedly suppressed TGF-β-induced IL-6 secretion from HFCs. Moreover, these inhibitors suppressed IL-6 mRNA expression in response to TGF-β stimulation.

Conclusions: Our findings indicate that TGF-β induces IL-6 protein secretion and gene expression in HFCs through the activation of p38 or p44/42 MAP kinases. These results suggest a potential association between IL-6-mediated inflammatory response and tissue hypertrophy in LSS, and we provide insights into molecular targets for therapeutic interventions targeting LSS-related inflammation through our analysis of the MAP kinase pathway using HFCs.

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来源期刊
Asian Spine Journal
Asian Spine Journal ORTHOPEDICS-
CiteScore
5.10
自引率
4.30%
发文量
108
审稿时长
24 weeks
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