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Expression and function of wingless and frizzled homologs in rheumatoid arthritis

机译:无翅和翻毛同系物的表达和功能 类风湿关节炎

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摘要

Rheumatoid arthritis (RA) is accompanied by synovial inflammation, proliferation, and cartilage destruction. The reasons the activation of synovial fibroblasts often persists despite antiinflammatory therapy are not known. One possibility is that the synovial membrane becomes gradually repopulated with immature mesenchymal and bone marrow cells with altered properties. To explore this hypothesis, we have investigated the expression in RA synovial tissues of various embryonic growth factors from the wingless (wnt) and frizzled (fz) families, which have been implicated in cell-fate determination in both bone marrow progenitors and limb-bud mesenchyme. Reverse transcriptase–PCR analysis revealed expression of five wnt (wnt1, 5a, 10b, 11, and 13) and three fz (fz2, 5, and 7) isoforms in RA synovial tissues. Osteoarthritis synovial tissues expressed much less wnt5a and fz5. Northern blotting confirmed the overexpression of wnt5a and fz5 in RA synovial tissues, in comparison to a panel of normal adult tissues. Compared with normal synovial fibroblasts, cultured RA fibroblast-like synoviocytes expressed higher levels of IL-6, IL-8, and IL-15. Transfection of normal fibroblasts with a wnt5a expression vector reproduced this pattern of cytokine expression and stimulated IL-15 secretion. These results suggest that the unusual phenotypic properties of RA fibroblasts may be attributable partly to their replacement with primitive fibroblast-like synoviocytes with characteristics of immature bone marrow and mesenchymal cells. Clear delineation of the signaling pathway(s) initiated by the wnt5a/fz5 ligand–receptor pair in the RA synovium may yield new targets for therapeutic intervention.
机译:类风湿关节炎(RA)伴有滑膜发炎,增生和软骨破坏。尽管抗炎治疗,滑膜成纤维细胞活化仍持续的原因尚不清楚。一种可能性是滑膜被逐渐改变特性的未成熟间充质和骨髓细胞所填充。为了探索这一假设,我们研究了无翅(wnt)和卷曲的(fz)家族的各种胚胎生长因子在RA滑膜组织中的表达,这些因子与骨髓祖细胞和肢体芽细胞命运的确定有关。间质逆转录-PCR分析显示RA​​滑膜组织中有5种wnt(wnt1、5a,10b,11和13)和3种fz(fz2、5和7)亚型的表达。骨关节炎滑膜组织表达的wnt5a和fz5少得多。 Northern印迹证实过表达 RA滑膜组织中的wnt5a和fz5 与一组正常的成人组织比较。与正常相比 滑膜成纤维细胞,培养的RA成纤维样滑膜细胞 表达更高水平的IL-6,IL-8和IL-15。转染 wnt5a 表达载体的正常成纤维细胞 重现这种细胞因子表达模式并刺激IL-15 分泌。这些结果表明异常的表型特性 RA成纤维细胞的部分归因于 具有未成熟特征的原始成纤维细胞样滑膜细胞 骨髓和间质细胞。清晰描述信号 由 wnt5a / fz5 发起的途径 RA滑膜中的配体-受体对可能产生新的靶标 治疗干预。

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