糖皮质激素通过抑制内源性PGE的产生来增强成纤维细胞介导的胶原凝胶收缩。

C M Sköld, X D Liu, Y K Zhu, T Umino, K Takigawa, Y Ohkuni, R F Ertl, J R Spurzem, D J Romberger, R Brattsand, S I Rennard
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引用次数: 35

摘要

糖皮质激素目前被认为是治疗炎症性气道和肺部疾病的首选药物,然而,它们在炎症的纤维化期并非常规有效。在目前的研究中,糖皮质激素被研究了其影响成纤维细胞介导的三维胶原凝胶收缩的能力,这是组织重塑的一个方面。地塞米松、布地奈德、氢化可的松和丙酸氟替卡松均能以浓度依赖的方式显著增强成纤维细胞的收缩力。糖皮质激素对支气管、皮肤和骨髓成纤维细胞介导的胶原凝胶收缩也有增强作用。收缩性的增加不是由于细胞增殖或胶原蛋白降解,因为糖皮质激素并没有改变凝胶中DNA和羟脯氨酸的数量。糖皮质激素处理的凝胶与对照凝胶相比,上清培养基中前列腺素E2 (PGE2)浓度较低。与此一致的是,在培养系统中添加外源性PGE2恢复了收缩特性,吲哚美辛增强了收缩,类似于糖皮质激素,这表明抑制前列腺素或相关的二十烷类化合物可能是收缩性增加的机制。DBcAMP、福斯克林和长效β 2激动剂福莫特罗能够逆转糖皮质激素对成纤维细胞介导的胶原凝胶收缩的影响,这表明cAMP增强剂可以抵消糖皮质激素的作用。因此,我们提供的证据表明,糖皮质激素能够通过抑制成纤维细胞内源性PGE合成直接增强成纤维细胞的收缩能力。这一发现可能是解释糖皮质激素在纤维化疾病晚期治疗效果不佳的一种可能机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Glucocorticoids augment fibroblast-mediated contraction of collagen gels by inhibition of endogenous PGE production.

Glucocorticoids are currently regarded as the drug of choice in the treatment of inflammatory airway and lung diseases, however, they are not routinely effective in fibrotic phases of inflammation. In the current study, glucocorticoids were investigated for their ability to affect fibroblast mediated contraction of a three dimensional collagen gel, a measure of one aspect of tissue remodeling. Dexamethasone, budesonide, hydrocortisone and fluticasone propionate were all able to significantly augment fibroblast contractility in a concentration dependent manner. Glucocorticoids also had an augmentative effect on collagen gel contraction mediated by fibroblasts from bronchi, skin and bone marrow. The increased contractility was not due to cell proliferation or to collagen degradation, since the glucocorticoids did not alter the amounts of DNA and hydroxyproline in the gels. The concentration of prostaglandin E2 (PGE2) in supernatant media was lower from glucocorticoid-treated gels compared to control gels. Consistent with this, addition of exogenous PGE2 to the culture system restored the contractile properties and indomethacin augmented contraction similar to the glucocorticoids suggesting that inhibition of prostaglandins or related eicosanoids may be the mechanism by which the increased contractility occurs. DBcAMP, forskolin and the long lasting beta2-agonist formoterol were able to reverse the effect of the glucocorticoids on fibroblast mediated collagen gel contraction suggesting that enhancers of cAMP can counteract the effect of glucocorticoids. Thus, we provide evidence that glucocorticoids have the ability to directly augment fibroblast contractility by inhibiting fibroblast endogenous PGE synthesis. The findings could be one possible mechanism to explain the poor therapeutic response to glucocorticoids on the later stages of fibrotic diseases.

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