首页> 外文期刊>Journal of orthopaedic research >Glucocorticoids inhibit tenocyte proliferation and Tendon progenitor cell recruitment.
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Glucocorticoids inhibit tenocyte proliferation and Tendon progenitor cell recruitment.

机译:糖皮质激素抑制肌腱细胞增殖和肌腱祖细胞募集。

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Corticosteroid injection is commonly used to treat tendon injuries but is often associated with tendon rupture and impaired tendon healing. The effects of dexamethasone on tenocytes have been studied in vitro but only using high concentrations of dexamethasone in monolayer cultures of tenocytes over short periods of time. We have therefore investigated the effects of physiological and pharmacological concentrations of dexamethasone on monolayer cultures of tenocytes over extended time periods. We have also used fibroblastic-colony forming unit cultures to examine the effects of dexamethasone on a progenitor cell population located in tendons. Culturing tenocytes in the presence of dexamethasone for a period of 24 days resulted in a concentration-related decrease in cell number and collagen synthesis as compared to control cultures. This effect was time dependent with cell number in both dexamethasone-treated and control cultures leveling off after 14 days with the control cultures reaching higher cell densities. In contrast in control cultures, collagen accumulation continued to increase until week 4, whereas in the presence of dexamethasone, this tended to level off after 14 days. To study the role of progenitor cell recruitment, the effects of dexamethasone were investigated using the fibroblastic-colony forming unit assay. Treatment with dexamethasone at concentrations of 0.1 nM to 10 microM leads to a progressive reduction in mean colony size as compared to control cultures. Colony number remained constant at concentrations below 10 nM but fell progressively at concentrations above this. In conclusion, dexamethasone reduces both cell number and collagen synthesis in tenocyte cultures in a concentration-dependent manner by both direct effects on tenocyte proliferation and collagen accumulation, and also by modulating the recruitment of tendon progenitor cells.
机译:皮质类固醇注射通常用于治疗肌腱损伤,但通常与肌腱破裂和肌腱愈合受损有关。已经在体外研究了地塞米松对肌腱细胞的作用,但仅在短时间内在肌腱细胞的单层培养中使用高浓度地塞米松。因此,我们研究了地塞米松的生理和药理浓度对延长时间的单核细胞单层培养的影响。我们还使用了成纤维细胞集落形成单位培养来检查地塞米松对位于肌腱中的祖细胞群的影响。与对照培养相比,在地塞米松存在下培养肌腱细胞24天会导致细胞数量和胶原蛋白合成的浓度相关下降。 14天后,地塞米松处理和对照培养物中的细胞数量趋于稳定,而对照培养物达到更高的细胞密度,这种作用随时间而变。相反,在对照培养物中,胶原蛋白的积累持续增加直到第4周,而在存在地塞米松的情况下,胶原蛋白的积累在14天后趋于稳定。为了研究祖细胞募集的作用,使用成纤维细胞集落形成单位测定法研究了地塞米松的作用。与对照培养相比,地塞米松浓度为0.1 nM至10 microM的处理导致平均菌落大小逐渐减少。浓度低于10 nM时菌落数保持恒定,但浓度高于10 nM时菌落数逐渐下降。总之,地塞米松通过直接作用于肌腱细胞增殖和胶原蛋白积累,以及通过调节肌腱祖细胞的募集,以浓度依赖的方式减少肌腱细胞培养物中的细胞数量和胶原蛋白合成。

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