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脱氢表雄酮在体外对成骨细胞代谢和IL-1β的影响
Effects of Dehydroepiandrosterone on Metabolism of Rat Osteoblasts and IL-1β in Vitro
【摘要】 目的探讨脱氢表雄酮(dehydroepiandrosterone,DHEA)对离体大鼠成骨细胞和IL-1β的影响。方法体外分离培养大鼠成骨细胞,取传一代细胞,分别给予10-5mmol/L、10-7mmol/L、10-9mmol/L DHEA培养72h,以10-8mmol/L雌二醇(estradiol,E2)为阳性对照,另设空白对照组。碱性磷酸酶(alkaline phosphatase,ALP)染色鉴定成骨细胞,MTT法检测成骨细胞的增殖能力,PNPP法测定ALP活性。ELISA法测定不同浓度DHEA培养液中IL-1β的水平。结果不同浓度DHEA组成骨细胞增殖能力和ALP的活性均有上升,其中以10-7mmol/L DHEA组最显著(P<0.01),其作用和E2相似(P>0.05);10-9mmol/L DHEA组单位细胞数的ALP活性高于空白对照组(P<0.05)。不同浓度的DHEA组IL-1β呈下降趋势,成骨细胞增殖能力及ALP活性和IL-1β成负相关。结论DHEA在体外促进大鼠成骨细胞生长和增殖,提高ALP活性,其作用可能和抑制IL-1β有关。
【Abstract】 Objective To investigate the effects of dehydroepiandrosterone(DHEA)on rat osteoblasts and IL-1β in vitro.Methods Rat’s osteoblasts were separated and cultured in vitro.Osteoblasts of first generation were treated with DHEA in different concentration(10-5,10-7,10-9mmol/L)for 72 hours,E2 in 10-8mmol/l was adopted as positive control group,and blank control group was also set up.The biological characteristics of osteoblasts were evaluated by phase-contrast microscopy and alkaline phosphatase(ALP)histochemistry.Proliferation ability of osteoblasts was examined by MTT,activity of ALP was determined by PNPP.Level of IL-1β in DHEA culture solution was determined by ELISA simultaneously.Results Proliferation and ALP activity of osteoblasts treated with DHEA in different concentration were raised,especially treated with DHEA in 10-7mmol/l(P<0.01),which was similar to E2(P>0.05).ALP activity of unitary cell population treated with DHEA in 10-9mmol/l was higher than blank control group(P<0.05).Downtrend of IL-1β could be seen in each DHEA group,and negative correlation between proliferation ability or ALP activity of OBs and IL-1β could also be found.Conclusion DHEA could stimulate proliferation and raise ALP activity of rat’s osteoblasts in vitro,whose mechanism might inhabit the expression of IL-1β.
【Key words】 Dehydroepiandrosterone; Osteoblasts; Cell Proliferation; Interleukin;
- 【文献出处】 脊柱外科杂志 ,Journal of Spinal Surgery , 编辑部邮箱 ,2008年02期
- 【分类号】R96
- 【下载频次】63