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首页> 外文期刊>International immunopharmacology >Fatty acids isolated from royal jelly modulate dendritic cell-mediated immune response in vitro.
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Fatty acids isolated from royal jelly modulate dendritic cell-mediated immune response in vitro.

机译:从蜂王浆中分离出的脂肪酸可在体外调节树突状细胞介导的免疫反应。

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Royal jelly (RJ), especially its protein components, has been shown to possess immunomodulatory activity. However, almost nothing is known about the influence of RJ fatty acids on the immune system. In this work we studied the effect of 10-hydroxy-2-decanoic acid (10-HDA) and 3,10-dihydroxy-decanoic acid (3,10-DDA), isolated from RJ, on the immune response using a model of rat dendritic cell (DC)-T-cell cocultures. Both fatty acids, at higher concentrations, inhibited the proliferation of allogeneic T cells. The effect of 10-HDA was stronger and was followed by a decrease in interleukin-2 (IL-2) production and down-regulation of IL-2 receptor expression. Spleen DC, cultivated with 10 mug/ml of fatty acids down-regulated the expression of CD86 and the production of IL-12, but up-regulated the production of IL-10. In contrast, DC, pretreated with 100 mug/ml of 3,10-DDA, up-regulated the expression of CD86 and augmented the proliferation of allogeneic T cells. The highest dose (200 mug/ml) of both fatty acids which was non-apoptotic for both T cells and DC, down-regulated the expression of MHC class II and CD86, decreased the production of IL-12 and made these DC less allostimulatory. The immunosuppressive activity of 3,10-DDA was also confirmed in vivo, using a model of Keyhole lymphet hemocyanine immunization of rats. In conclusion, our results showed the immunomodulatory activity of RJ fatty acids and suggest that DC are a significant target of their action.
机译:蜂王浆(RJ),特别是其蛋白质成分,已显示具有免疫调节活性。但是,关于RJ脂肪酸对免疫系统的影响几乎一无所知。在这项工作中,我们使用以下模型研究了从RJ中分离出的10-羟基-2-癸酸(10-HDA)和3,10-二羟基癸酸(3,10-DDA)对免疫反应的影响。大鼠树突状细胞(DC)-T细胞共培养。两种脂肪酸都以较高的浓度抑制同种异体T细胞的增殖。 10-HDA的作用更强,其后是白介素2(IL-2)产生的减少和IL-2受体表达的下调。用10杯/毫升脂肪酸培养的脾脏DC下调CD86的表达和IL-12的产生,但上调IL-10的产生。相反,用100杯/毫升的3,10-DDA预处理的DC上调CD86的表达并增强同种异体T细胞的增殖。两种脂肪酸的最高剂量(200杯/毫升)对T细胞和DC均不凋亡,下调MHC II类和CD86的表达,降低IL-12的产生,并使这些DC的同种异体刺激性降低。还使用大鼠Keyhole淋巴血蓝蛋白免疫模型在体内证实了3,10-DDA的免疫抑制活性。总之,我们的结果显示了RJ脂肪酸的免疫调节活性,并表明DC是其作用的重要靶标。

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