首页> 美国卫生研究院文献>British Journal of Cancer >Verapamil sensitizes normal and neoplastic rodent intestinal tissues to the stathmokinetic effect of vincristine in vivo.
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Verapamil sensitizes normal and neoplastic rodent intestinal tissues to the stathmokinetic effect of vincristine in vivo.

机译:维拉帕米可使正常和赘生性啮齿动物肠道组织对长春新碱在体内的运动动力学效应敏感。

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摘要

A morphological method has been developed allowing measurement of the effect on intestinal epithelia of vincristine. In routinely prepared tissue sections the proportion of mitotic events progressing beyond metaphase is counted by microscopy. When estimated over a range of doses of vincristine this post-metaphase index (PMI) can be used to compare the sensitivity of differing intact tissues. Intestinal tumours were induced in rats by chemical carcinogenesis. Administration of vincristine in the presence or absence of verapamil was performed in these tumour-bearing animals. Sections were prepared from colonic and small-bowel tumours and from normal mucosa. The results show that verapamil increases the sensitivity of the tissues studied to vincristine. A dose dependent effect of verapamil on vincristine sensitisation was demonstrated in colonic tissues. These findings indicate a shared pharmacological property between the resistance of primary tumour tissue and the multidrug-resistance phenotype.
机译:已经开发出一种形态学方法,其允许测量对长春新碱的肠上皮细胞的作用。在常规制备的组织切片中,通过显微镜计数有丝分裂事件超过中期的比例。当估计长春新碱的剂量范围时,该中期后指数(PMI)可用于比较不同完整组织的敏感性。通过化学致癌作用在大鼠中诱发肠肿瘤。在这些荷瘤动物中,在存在或不存在维拉帕米的情况下进行长春新碱的给药。从结肠和小肠肿瘤以及正常粘膜制备切片。结果表明,维拉帕米可提高所研究组织对长春新碱的敏感性。维拉帕米对长春新碱致敏的剂量依赖性效应在结肠组织中得到证实。这些发现表明原发肿瘤组织的耐药性与多药耐药性表型之间具有共同的药理特性。

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