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首页> 美国卫生研究院文献>Clinical and Experimental Immunology >Anti-inflammatory effect of Viscum album agglutinin-I (VAA-I): induction of apoptosis in activated neutrophils and inhibition of lipopolysaccharide-induced neutrophilic inflammation in vivo
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Anti-inflammatory effect of Viscum album agglutinin-I (VAA-I): induction of apoptosis in activated neutrophils and inhibition of lipopolysaccharide-induced neutrophilic inflammation in vivo

机译:Viscum album agglutinin-I(VAA-I)的抗炎作用:在体内激活中性粒细胞诱导凋亡并抑制脂多糖诱导的中性粒细胞炎症

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Viscum album agglutinin-I (VAA-I) is a plant lectin which possesses antitumoral properties. This lectin is also known for its immunostimulatory effects when used at low concentrations (1–100 ng/ml). We have demonstrated recently that VAA-I is a potent inducer of human neutrophil apoptosis in vitro when used at higher concentrations. The role of VAA-I on activated neutrophils has not so far been investigated and its potential proinflammatory properties in vivo are poorly documented. Herein, we demonstrated that VAA-I (1000 ng/ml) induces apoptosis in lipopolysaccharide (LPS)-treated human neutrophils in vitro as well as in murine neutrophils isolated from lipopolysaccharide (LPS)-induced neutrophil influx. Using this model, we found that administration of VAA-I (100 or 1000 ng/ml) did not induce an inflammatory response. However, when used at 1 or 10 ng/ml, VAA-I was found to significantly induce a transitory inflammatory response, based on an increased leucocyte infiltration (>98% neutrophils). Also, we found that VAA-I inhibits LPS-induced neutrophil influx when administered simultaneously with LPS. In such conditions, some characteristic apoptotic neutrophils were observed in the pouch. Unlike LPS, which increased the production of some cytokines, VAA-I (1 or 10 ng/ml) did not increase the production of tumour necrosis factor (TNF)-α, interleukin (IL)-1Ra, IL-1α, IL-β, IL-8, IL-10 or IL-12 (p70) in human neutrophils. We conclude that VAA-I possesses the ability to induce apoptosis of preactivated neutrophils at a concentration that does not induce a proinflammatory response. Moreover, we conclude that VAA-I can inhibit a LPS-induced proinflammatory response in vivo. These data may provide new clinical perspectives in future mistletoe therapy and favour its potential utilization based on anti-inflammatory activity that at first appears contradictory with its use as immunostimulant.
机译:Viscum Album Agglutinin-I(VAA-I)是一种具有抗肿瘤特性的植物凝集素。当以低浓度(1–100 ng / ml)使用时,这种凝集素也以其免疫刺激作用而闻名。最近我们证明,当以较高浓度使用时,VAA-1是体外人嗜中性粒细胞凋亡的有效诱导剂。迄今为止,尚未研究VAA-1在活化的中性粒细胞中的作用,并且其体内潜在的促炎性质尚未得到充分记录。本文中,我们证明了VAA-1(1000 ng / ml)体外诱导脂多糖(LPS)处理的人中性粒细胞以及从脂多糖(LPS)诱导的中性粒细胞流入中分离出的鼠中性粒细胞凋亡。使用该模型,我们发现施用VAA-1(100或1000 ng / ml)不会引起炎症反应。但是,当以1 ng / ml或10 ng / ml的量使用时,VAA-1被发现会基于白细胞浸润的增加(> 98%的中性粒细胞)显着诱导短暂的炎症反应。而且,我们发现当与LPS同时给药时,VAA-1抑制LPS诱导的中性粒细胞流入。在这种情况下,在袋中观察到一些特征性凋亡中性粒细胞。与LPS会增加某些细胞因子的产生不同,VAA-1(1或10 ng / ml)不会增加肿瘤坏死因子(TNF)-α,白介素(IL)-1Ra,IL-1α,IL-人中性粒细胞中的β,IL-8,IL-10或IL-12(p70)。我们得出结论,VAA-1具有在不诱导促炎反应的浓度下诱导预活化嗜中性白细胞凋亡的能力。此外,我们得出结论,VAA-1可以在体内抑制LPS诱导的促炎反应。这些数据可能为未来的槲寄生疗法提供新的临床观点,并基于其最初作为其免疫刺激剂的使用而产生的抗炎活性,有利于其潜在的利用。

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