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首页> 外文期刊>Bioscience Reports >Verotoxin/Globotriaosyl Ceramide Recognition: Angiopathy, Angiogenesis and Antineoplasia
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Verotoxin/Globotriaosyl Ceramide Recognition: Angiopathy, Angiogenesis and Antineoplasia

机译:Verotoxin / Globotriaosyl神经酰胺的识别:血管病,血管生成和抗neosoplasia

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摘要

Verotoxin (VT) is involved in the etiology of both hemorrhagic colitis and the hemolytic uremic syndrome which are microvasculopathies of the colon and pediatric renal glomerulus respectively. Thus, VT can be considered a vasotoxin. Cell sensitivity in vitro varies according to the receptor glycolipid (globotriaosyl ceramide-Gb_3) expression and also to intracellular trafficking of the receptor/toxin complex, such that in highly sensitive cells, the toxin is targeted to the endoplasmic reticulum and nuclear envelope. Such cells include tumor cells which have become drug resistant. Thus Gb_3 is upregulated in certain tumors and when such tumor cells become drug resistant, their sensitivity to verotoxin increases. This may be due to a direct role of the MDR1 drug efflux pump in glycolipid biosynthesis, In addition to the tumor tissue, the toxin receptor may also be expressed in the tumor neovasculature suggesting that activated endothelial cells may be verotoxin sensitive. Thus VT may have both a direct and indirect antineoplastic potential. VT has proved highly effective in a xenograft cancer model and the possible therapeutic use of VT is discussed.
机译:Verotoxin(VT)参与出血性结肠炎和溶血性尿毒症综合征的病因,溶血性尿毒症综合征分别是结肠和小儿肾小球的微血管病变。因此,VT可以被认为是一种血管毒素。体外细胞敏感性根据受体糖脂(globotriaosyl ceramide-Gb_3)的表达以及受体/毒素复合物的细胞内运输而变化,从而在高度敏感的细胞中,毒素靶向内质网和核被膜。这样的细胞包括已经变成抗药性的肿瘤细胞。因此,Gb_3在某些肿瘤中被上调,并且当这种肿瘤细胞变得耐药时,它们对维毒素的敏感性增加。这可能是由于MDR1药物外排泵在糖脂生物合成中的直接作用。除肿瘤组织外,毒素受体也可能在肿瘤新脉管系统中表达,这表明活化的内皮细胞可能对维罗毒素敏感。因此,VT可能同时具有直接和间接的抗肿瘤潜力。 VT已被证明在异种移植癌模型中非常有效,并讨论了VT的可能治疗用途。

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