首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >1,25 (OH)(2) Vitamin D(3)-Stimulated Osteoclast Formation in Spleen-Osteoblast Cocultures Is Mediated in Part by Enhanced IL-1alpha and Receptor Activator of NF-kappaB Ligand Production in Osteoblasts.
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1,25 (OH)(2) Vitamin D(3)-Stimulated Osteoclast Formation in Spleen-Osteoblast Cocultures Is Mediated in Part by Enhanced IL-1alpha and Receptor Activator of NF-kappaB Ligand Production in Osteoblasts.

机译:脾-成骨细胞共培养物中的1,25(OH)(2)维生素D(3)刺激的破骨细胞形成部分由成骨细胞中增强的IL-1α和NF-κB配体的受体激活剂介导。

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We examined the ability of 1,25 (OH)(2) vitamin D(3) (Vit D) to stimulate osteoclast-like cell (OCL) formation in cocultures of spleen cells and primary calvarial osteoblasts from wild-type (WT) and IL-1R type 1-deficient (knockout; KO) mice. Vit D dose dependently increased OCL in cocultures containing WT osteoblasts. In contrast, there was a 90% reduction in OCL numbers in cocultures containing KO osteoblasts. In cocultures with either WT or KO osteoblasts, treatment with Vit D increased receptor activator of NF-kappaB ligand mRNA by 17-, 19-, or 3.5-fold, respectively. Vit D decreased osteoprotegerin mRNA to undetectable in all groups. Intracellular IL-1alpha protein increased after Vit D treatment in cocultures containing WT, but not KO osteoblasts. We also examined direct effects of Vit D, IL-1alpha, and their combination on gene expression in primary osteoblasts. In WT cells, Vit D and IL-1 stimulated receptor activator of NF-kappaB ligand mRNA expression by 3- and 4-fold, respectively, and their combination produced a 7-fold increase. Inhibition of osteoprotegerin mRNA in WT cells was partial with either agent alone and greatest with their combination. In KO cells, only Vit D stimulated a response. IL-1 alone increased IL-1alpha protein expression in WT osteoblasts. However, in combination with Vit D, there was a synergistic response (100-fold increase). In KO cultures, there were no effects of IL-1, Vit D, or their combination on IL-1alpha protein. These results demonstrate interactions between IL-1 and Vit D in primary osteoblasts that appear important in both regulation of IL-1alpha production and the ability of Vit D to support osteoclastogenesis.
机译:我们研究了在野生型(WT)和脾脏和原发颅盖骨成骨细胞共培养中1,25(OH)(2)维生素D(3)(维生素D)刺激破骨细胞样细胞(OCL)形成的能力。 IL-1R 1型缺陷(敲除; KO)小鼠。 Vit D在含有WT成骨细胞的共培养物中剂量依赖性地增加OCL。相反,在含有KO成骨细胞的共培养物中,OCL数减少了90%。与WT或KO成骨细胞共培养时,用Vit D处理可使NF-κB配体mRNA的受体激活剂分别增加17倍,19倍或3.5倍。 Vit D将骨保护素mRNA降低至所有组均无法检测。 Vit D处理后,在含有WT但不含KO成骨细胞的共培养物中,细胞内IL-1α蛋白增加。我们还检查了Vit D,IL-1alpha及其组合对原代成骨细胞基因表达的直接影响。在WT细胞中,Vit D和IL-1分别刺激NF-κB配体mRNA表达的受体激活子增加了3倍和4倍,并且它们的组合产生了7倍的增加。单独使用任何一种试剂对WT细胞中骨保护素mRNA的抑制作用部分,对它们的组合影响最大。在KO细胞中,只有Vit D刺激了反应。单独的IL-1可以增加WT成骨细胞中IL-1alpha蛋白的表达。但是,与Vit D结合使用时,会产生协同反应(增加100倍)。在KO培养物中,IL-1,Vit D或它们的组合对IL-1alpha蛋白没有影响。这些结果表明原代成骨细胞中IL-1和Vit D之间的相互作用在调节IL-1α的产生和Vit D支持破骨细胞形成的能力中都显得很重要。

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