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Androgen metabolism and inhibition of interleukin-1 synthesis in primary cultured human synovial macrophages

机译:原代培养的人滑膜巨噬细胞中雄激素代谢和白介素-1合成的抑制

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摘要

The presence of androgen receptors on synovial macrophages in human normal and rheumatoid synovial tissues has been described previously. It is now reported that primary cultured human macrophages obtained from normal and rheumatoid synovia express functional androgen receptors. We have investigated the capacity of cultured macrophages to metabolize androgens and have found that these cells were capable of metabolizing testosterone to the bioactive metabolite dihydrotestosterone. Therefore, macrophages contain the key enzymes of steroidogenesis, in particular the 5α-treductase. Furthermore, interleukin-1β production by primary cultured rheumatoid macrophages was analysed, following exposure to physiological concentrations of testosterone (10−8 M). A significant decrease of IL-1β levels in conditioned media after 24 h (p < 0.05) was observed. It is concluded that androgens may act directly on human macrophages and may interfere with some of their functions via receptor-dependent mechanisms.
机译:先前已经描述了人类正常和类风湿性滑膜组织中滑膜巨噬细胞上雄激素受体的存在。现在据报道,从正常和类风湿性滑膜中获得的原代培养的人类巨噬细胞表达功能性雄激素受体。我们研究了培养的巨噬细胞代谢雄激素的能力,并发现这些细胞能够将睾丸激素代谢为生物活性代谢物二氢睾丸激素。因此,巨噬细胞包含类固醇生成的关键酶,特别是5α-过氧化物酶。此外,在暴露于生理浓度的睾丸激素(10 -8 M)后,分析了原代培养的类风湿巨噬细胞产生的白介素-1β。 24小时后,条件培养基中的IL-1β水平显着下降(p <0.05)。结论是,雄激素可能直接作用于人类巨噬细胞,并可能通过受体依赖性机制干扰其某些功能。

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