首页> 美国卫生研究院文献>International Journal of Oncology >Methanolic extract of white asparagus shoots activates TRAIL apoptotic death pathway in human cancer cells and inhibits colon carcinogenesis in a preclinical model
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Methanolic extract of white asparagus shoots activates TRAIL apoptotic death pathway in human cancer cells and inhibits colon carcinogenesis in a preclinical model

机译:在临床前模型中白芦笋芽的甲醇提取物激活人癌细胞中的TRAIL凋亡死亡途径并抑制结肠癌的发生。

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摘要

Shoots of white asparagus are a popular vegetable dish, known to be rich in many bioactive phytochemicals reported to possess antioxidant, and anti-inflammatory and antitumor activities. We evaluated the anticancer mechanisms of a methanolic extract of Asparagus officinalis L. shoots (Asp) on human colon carcinoma cells (SW480) and their derived metastatic cells (SW620), and Asp chemopreventive properties were also assessed in a model of colon carcinogenesis. SW480 and SW620 cell proliferation was inhibited by 80% after exposure to Asp (80 μg/ml). We demonstrated that Asp induced cell death through the activation of TRAIL DR4/DR5 death receptors leading to the activation of caspase-8 and caspase-3 and to cell apoptosis. By specific blocking agents of DR4/DR5 receptors we were able to prevent Asp-triggered cell death confirming the key role of DR4/DR5 receptors. We found also that Asp (80 μg/ml) was able to potentiate the effects of the cytokine TRAIL on cell death even in the TRAIL-resistant metastatic SW620 cells. Colon carcinogenesis was initiated in Wistar rats by intraperitoneal injections of azoxymethane (AOM), once a week for two weeks. One week after (post-initiation) rats received daily Asp (0.01%, 14 mg/kg body weight) in drinking water. After 7 weeks of Asp-treatment the colon of rats exhibited a 50% reduction of the number of preneoplastic lesions (aberrant crypt foci). In addition Asp induced inhibition of several pro-inflammatory mediators, in association with an increased expression of host-defense mediators. In the colonic mucosa of Asp-treated rats we also confirmed the pro-apoptotic effects observed in vitro including the activation of the TRAIL death-receptor signaling pathway. Taken together, our data highlight the chemopreventive effects of Asp on colon carcinogenesis and its ability to promote normal cellular homeostasis.
机译:白芦笋的芽是一种流行的蔬菜,据称富含许多据称具有抗氧化剂,抗炎和抗肿瘤活性的生物活性植物化学物质。我们评估了芦笋茎(Asp)的甲醇提取物对人结肠癌细胞(SW480)及其衍生的转移细胞(SW620)的抗癌机制,并且还在结肠癌发生模型中评估了Asp的化学预防特性。暴露于Asp(80μg/ ml)后,SW480和SW620细胞增殖被抑制了80%。我们证明Asp通过TRAIL DR4 / DR5死亡受体的激活诱导细胞死亡,从而导致caspase-8和caspase-3的激活以及细胞凋亡。通过DR4 / DR5受体的特异性阻断剂,我们能够预防Asp触发的细胞死亡,从而证实了DR4 / DR5受体的关键作用。我们还发现,即使在对TRAIL耐药的转移性SW620细胞中,Asp(80μg/ ml)能够增强细胞因子TRAIL对细胞死亡的影响。 Wistar大鼠通过每周一次腹膜内注射乙氧基甲烷(AOM)引发结肠癌变,持续两周。 (起始后)一周后,大鼠每天接受饮用水中的Asp(0.01%,14 mg / kg体重)。 Asp处理7周后,大鼠结肠的肿瘤前病变(异常隐窝灶)数量减少了50%。另外,Asp诱导了几种促炎性介质的抑制,与宿主防御介质的表达增加有关。在经Asp处理的大鼠的结肠粘膜中,我们还证实了在体外观察到的促凋亡作用,包括激活TRAIL死亡受体信号通路。综上所述,我们的数据突出了Asp对结肠癌发生的化学预防作用及其促进正常细胞稳态的能力。

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