Formula-Pattern Research Center, School of Traditional Chinese Medicine, Jinan University, 510632, Guangzhou, China.
Chinese Medicine Department, South China Agricultural University Hospital, 510642, Guangzhou, China.
Phytomedicine. 2022 Dec;107:154479. doi: 10.1016/j.phymed.2022.154479. Epub 2022 Sep 29.
Rheumatoid arthritis (RA), the most common type of inflammatory arthritis, can cause bone damage and disability. Triptolide, a prominent treatment for RA, has satisfactory anti-inflammatory effects. However, the mechanism of action of triptolide in RA remains unknown.
This study aimed to explore the molecular mechanisms underlying triptolide-mediated improvements in RA and identify the miRNA pathway responsible for these effects.
We identified various dysregulated miRNAs associated with RA by mining previously described microarray data and verified and screened these candidates using RT-qPCR. Hematoxylin-eosin staining was then applied to identify pathological changes in the affected joints, and cell counting kit-8 analysis and flow cytometry were employed to examine cell proliferation and apoptosis, respectively. Extracted exosomes were verified using transmission electron microscopy.
Our results revealed that the legs of rats with collagen-induced arthritis presented with obvious swelling and bone damage, a high degree of inflammatory cell infiltration into the synovium, and structural changes to the cartilage. Data mining identified 39 dysregulated miRNAs in these tissues, and RT-qPCR further refined these observations to highlight miR-221 as a potential RA biomarker. Subsequent evaluations revealed that fibroblast-like synovial (FLS) cells secrete Exs carrying dysregulated miR-221 in vitro. These Exs mediate miR-221 levels, inflammation, and TLR4/MyD88 signaling via their fusion with chondrocytes, leading to changes in chondrocyte growth and metabolic factor levels. Additionally, the addition of triptolide impaired miR-221 expression, cell proliferation, inflammatory factors, and the protein levels of TLR4/MyD88 in RA-FLS and promoted the apoptosis of FLS. The therapeutic effect of triptolide on miR-221 Exs was reversed by miR-221 inhibitor in both normal and RA FLS.
Our research shows that effective treatment with triptolide is mediated by its regulation of growth and secretory functions of chondrocytes via the inhibition of miR-221 secretion by FLS, providing a new target and natural medicinal candidate for future RA treatments.
类风湿关节炎(RA)是最常见的炎症性关节炎类型,可导致骨损伤和残疾。雷公藤红素是治疗 RA 的一种突出药物,具有令人满意的抗炎作用。然而,雷公藤红素治疗 RA 的作用机制尚不清楚。
本研究旨在探讨雷公藤红素介导的 RA 改善的分子机制,并确定负责这些效果的 miRNA 途径。
我们通过挖掘先前描述的微阵列数据来鉴定与 RA 相关的各种失调 miRNA,并使用 RT-qPCR 对这些候选物进行验证和筛选。苏木精-伊红染色用于鉴定受影响关节的病理变化,细胞计数试剂盒-8 分析和流式细胞术分别用于检查细胞增殖和凋亡。通过透射电子显微镜验证提取的外泌体。
我们的结果表明,胶原诱导性关节炎大鼠的腿部出现明显肿胀和骨损伤,滑膜中有大量炎性细胞浸润,软骨结构发生变化。数据挖掘鉴定出这些组织中有 39 个失调 miRNA,RT-qPCR 进一步对这些观察结果进行了细化,突出了 miR-221 作为潜在的 RA 生物标志物。随后的评估表明,成纤维样滑膜(FLS)细胞在体外分泌携带失调 miR-221 的 Exs。这些 Exs 通过与软骨细胞融合来调节 miR-221 水平、炎症和 TLR4/MyD88 信号,导致软骨细胞生长和代谢因子水平的变化。此外,雷公藤红素的添加可损害 RA-FLS 中 miR-221 的表达、细胞增殖、炎症因子和 TLR4/MyD88 的蛋白水平,并促进 FLS 的凋亡。在正常和 RA FLS 中,miR-221 抑制剂逆转了雷公藤红素对 miR-221 Exs 的治疗作用。
我们的研究表明,雷公藤红素的有效治疗是通过其抑制 FLS 中 miR-221 的分泌来调节软骨细胞的生长和分泌功能介导的,为未来的 RA 治疗提供了新的靶点和天然药物候选物。
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