类风湿关节炎滑膜细胞中糖皮质激素再激活能力降低：交感神经系统的潜在作用？

Reduced capacity for the reactivation of glucocorticoids in rheumatoid arthritis synovial cells: possible role of the sympathetic nervous system?

作者信息

Schmidt Martin, Weidler Claudia, Naumann Heidrun, Anders Sven, Schölmerich Jürgen, Straub Rainer H

机构信息

Hospital of the Friedrich-Schiller-University, Jena, Germany.

出版信息

Arthritis Rheum. 2005 Jun;52(6):1711-20. doi: 10.1002/art.21091.

DOI:10.1002/art.21091

PMID:15934114

Abstract

OBJECTIVE

Cortisol, the biologically active glucocorticoid, is a major endogenous antiinflammatory factor in rheumatoid arthritis (RA). The aim of this study was to examine the local conversion of cortisol to biologically inactive cortisone and vice versa (the cortisol-cortisone shuttle) in RA and osteoarthritis (OA) patients.

METHODS

Thin-layer chromatography and phosphorimaging were used to examine the cortisol-cortisone shuttle in mixed synovial cells. Double immunohistochemistry was used to assess the key enzymes 11beta-hydroxysteroid dehydrogenase 1 (11beta-HSD1) and 11beta-HSD2 and their possible cellular locations.

RESULTS

Double immunohistochemistry demonstrated 11beta-HSD1/2+ macrophages in the sublining area. The ratio of 11beta-HSD2+ cells to 11beta-HSD1+ cells was significantly higher in RA than in OA patients. Cortisol was converted to inactive cortisone in mixed synovial cells from RA and OA patients, which was largely inhibited by carbenoxolone (11beta-HSD1 and 11beta-HSD2 inhibitor). Using metyrapone to inhibit the 11beta-HSD1 reducing reaction (cortisone --> cortisol), we demonstrated that the capacity for reactivation of cortisone to cortisol was significantly higher in OA than in RA patients. Although the capacity for the cortisone-cortisol shuttle was higher in synovial cells from less-inflamed OA tissue compared with inflamed RA tissue, it was obvious that synovial inflammation in RA, but not OA, was related positively to the reactivation of cortisone. This indicates that in RA, a cause other than typical inflammatory factors inhibits the reactivation of cortisone. Since isoproterenol and adenosine inhibited the cortisol-cortisone shuttle, the loss of sympathetic nerve fibers (loss of beta-adrenergic agonist and adenosine) may be the missing link that accounts for the increased cortisol-cortisone shuttle in RA.

CONCLUSION

This study demonstrates a reduced capacity for local reactivation of cortisone in RA synovial cells. Since synthetic glucocorticoids also use this reactivation shuttle, the results also apply to therapeutic glucocorticoids. This defective reactivation of cortisone may be an important unrecognized pathophysiologic factor in RA.

摘要

目的

皮质醇作为具有生物活性的糖皮质激素，是类风湿关节炎（RA）中主要的内源性抗炎因子。本研究旨在检测RA和骨关节炎（OA）患者体内皮质醇向生物活性缺失的可的松的局部转化情况，以及反之（皮质醇 - 可的松穿梭）的转化情况。

方法

采用薄层色谱法和磷成像技术检测混合滑膜细胞中的皮质醇 - 可的松穿梭情况。运用双重免疫组织化学法评估关键酶11β - 羟基类固醇脱氢酶1（11β - HSD1）和11β - 羟基类固醇脱氢酶2（11β - HSD2）及其可能的细胞定位。

结果

双重免疫组织化学显示，在滑膜下层区域存在11β - HSD1/2 +巨噬细胞。RA患者中11β - HSD2 +细胞与11β - HSD1 +细胞的比例显著高于OA患者。RA和OA患者的混合滑膜细胞中，皮质醇会转化为无活性的可的松，而这种转化在很大程度上受到甘珀酸（11β - HSD1和11β - HSD2抑制剂）的抑制。使用甲吡酮抑制11β - HSD1还原反应（可的松→皮质醇），我们发现OA患者可的松再激活为皮质醇的能力显著高于RA患者。尽管与炎症较重的RA组织相比，炎症较轻的OA组织的滑膜细胞中可的松 - 皮质醇穿梭能力更高，但很明显，RA而非OA中的滑膜炎症与可的松的再激活呈正相关。这表明在RA中，除了典型炎症因子之外的其他因素抑制了可的松的再激活。由于异丙肾上腺素和腺苷抑制皮质醇 - 可的松穿梭，交感神经纤维的缺失（β - 肾上腺素能激动剂和腺苷的缺失）可能是导致RA中皮质醇 - 可的松穿梭增加的缺失环节。