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首页> 外文期刊>Bone >IL-12 inhibits TNF-alpha induced osteoclastogenesis via a T cell-independent mechanism in vivo.
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IL-12 inhibits TNF-alpha induced osteoclastogenesis via a T cell-independent mechanism in vivo.

机译:IL-12在体内通过非T细胞依赖性机制抑制TNF-α诱导的破骨细胞生成。

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It has been reported that TNF-alpha plays an important role in bone resorption in pathological conditions. IL-12, which is a T cell mediator, is also an important inflammatory cytokine. We previously reported that IL-12 induces apoptosis in bone marrow cells treated with TNF-alpha in vitro via an interaction between TNF-alpha-induced Fas and IL-12-induced Fas ligand (FasL), and that, as a result, osteoclastogenesis is inhibited. The purpose of this study was to investigate the effects of IL-12 on TNF-alpha-mediated osteoclastogenesis in vivo. We administered TNF-alpha with and without IL-12 into the supracalvaria in mice. The numbers of osteoclasts in the sutures in the calvaria were higher in mice administered TNF-alpha than in control mice not administered TNF-alpha. The numbers of osteoclasts in mice administered both TNF-alpha and IL-12 were lower than those in mice administered only TNF-alpha. Next, we determined the levels of mRNAs for cathepsin K and tartrate-resistant acid phosphatase (TRAP). mRNA levels were increased in mice administered TNF-alpha compared with control mice, but not in mice administered both TNF-alpha and IL-12. We also evaluated the amounts of tartrate-resistant acid phosphatase 5b (TRACP 5b) in mouse sera. The levels of TRACP 5b in mice administered TNF-alpha were higher than those in control mice. On the other hand, in mice administered both TNF-alpha and IL-12, the levels were lower than those in mice administered TNF-alpha alone. Fas and FasL expression levels were analyzed by real-time RT-PCR. The levels of Fas mRNA were increased in the calvaria of mice administered TNF-alpha compared with control mice, while those of FasL mRNAs were increased in the calvaria of mice administered IL-12. In TdT-mediated dUTP-biotin nick end-labeling (TUNEL) assays, many apoptotic cells were found in the sutures in the calvaria of mice administered both TNF-alpha and IL-12. IL-12 also inhibited TNF-alpha-induced osteoclastogenesis in mice whose T cells were blocked by anti-CD4 and anti-CD8 antibodies. These results suggest that IL-12 inhibits TNF-alpha-mediated osteoclastogenesis and induces apoptotic changes through an interaction between TNF-alpha-induced Fas and IL-12-induced FasL, in vivo, via a T cell-independent mechanism.
机译:据报道,TNF-α在病理条件下的骨吸收中起重要作用。 IL-12是T细胞的介质,也是重要的炎症细胞因子。我们以前曾报道过,IL-12通过TNF-α诱导的Fas与IL-12诱导的Fas配体(FasL)之间的相互作用,在体外用TNF-α处理的骨髓细胞中诱导凋亡,结果是破骨细胞发生被禁止。本研究的目的是研究IL-12对体内TNF-α介导的破骨细胞形成的影响。我们在小鼠上睑静脉注射有和没有IL-12的TNF-α。给予TNF-α的小鼠颅骨缝线中破骨细胞的数量高于未给予TNF-α的对照小鼠。既施用TNF-α又施用IL-12的小鼠中的破骨细胞数量低于仅施用TNF-α的小鼠中的破骨细胞数量。接下来,我们确定了组织蛋白酶K和抗酒石酸酸性磷酸酶(TRAP)的mRNA的水平。与对照小鼠相比,施用TNF-α的小鼠的mRNA水平升高,但同时施用TNF-α和IL-12的小鼠却未升高。我们还评估了小鼠血清中抗酒石酸酸性磷酸酶5b(TRACP 5b)的量。给予TNF-α的小鼠中TRACP 5b的水平高于对照组小鼠。另一方面,在同时给予TNF-α和IL-12的小鼠中,该水平低于仅给予TNF-α的小鼠。通过实时RT-PCR分析Fas和FasL表达水平。与对照小鼠相比,给予TNF-α的小鼠的颅盖中Fas mRNA的水平升高,而给予IL-12的小鼠的颅盖中FasL mRNA的水平升高。在TdT介导的dUTP-生物素缺口末端标记(TUNEL)分析中,在同时施用TNF-α和IL-12的小鼠颅盖缝线中发现了许多凋亡细胞。 IL-12还抑制了其T细胞被抗CD4和抗CD8抗体阻断的小鼠中TNF-α诱导的破骨细胞生成。这些结果表明,IL-12在体内通过T细胞非依赖性机制,通过TNF-α诱导的Fas和IL-12诱导的FasL之间的相互作用抑制TNF-α介导的破骨细胞形成并诱导凋亡变化。

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