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人类关节软骨细胞中白细胞介素1受体的调控

Regulation of interleukin 1 receptors in human articular chondrocytes.

作者信息

McCollum R, Martel-Pelletier J, DiBattista J, Pelletier J P

机构信息

Rheumatic Diseases Unit Research Laboratory, Notre-Dame Hospital Research Center, Montreal, PQ, Canada.

出版信息

J Rheumatol Suppl. 1991 Feb;27:85-8.

PMID:1827502
Abstract

Interleukin 1 (IL-1) exerts pronounced effects on articular cartilage by increasing matrix molecule turnover and metalloprotease synthesis. These effects are believed to be mediated through a high affinity cell surface receptor (IL-1R) present on chondrocytes. Normal human chondrocytes express about 3,000-5,000 sites/cell. The downregulation of IL-1R could potentially reduce the biological effectiveness of IL-1 and as a result influence inflammatory conditions. Agents which modulate the number of IL-1R were investigated. Cytokines, such as IL-1 alpha (1 ng/ml) and IL-1 beta (1 ng/ml), were found to reduce the chondrocyte IL-1R level by about 78% versus the control. Other cytokines tested, IL-2 (20 ng/ml) and tumor necrosis factor-alpha (1 ng/ml), also reduced IL-1R levels but to a lesser extent; 52 and 69% inhibition were recorded, respectively. The growth factor bFGF (50 ng/ml) induced a 48% reduction versus the basal level, and a therapeutic dosage of indomethacin (1.5 micrograms/ml) elicited only a slight reduction (10%). Hydrocortisone had a variable effect on the IL-1R level.

摘要

白细胞介素1(IL-1)通过增加基质分子周转率和金属蛋白酶合成,对关节软骨产生显著影响。这些作用被认为是通过软骨细胞上存在的高亲和力细胞表面受体(IL-1R)介导的。正常人软骨细胞每个细胞表达约3000 - 5000个位点。IL-1R的下调可能会降低IL-1的生物学效应,从而影响炎症状态。对调节IL-1R数量的药物进行了研究。发现细胞因子,如IL-1α(1纳克/毫升)和IL-1β(1纳克/毫升),与对照组相比,可使软骨细胞IL-1R水平降低约78%。测试的其他细胞因子,IL-2(20纳克/毫升)和肿瘤坏死因子-α(1纳克/毫升),也降低了IL-1R水平,但程度较小;分别记录到52%和69%的抑制率。生长因子bFGF(50纳克/毫升)与基础水平相比,诱导降低了48%,而治疗剂量的吲哚美辛(1.5微克/毫升)仅引起轻微降低(10%)。氢化可的松对IL-1R水平有可变作用。

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