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体内给予长春新碱和美登素后P388小鼠白血病的流式微量荧光分析。

Flow microfluorometric analysis of P388 murine leukemia after administration of vincristine and maytansine in vivo.

作者信息

Alabaster O, Cassidy M

出版信息

J Natl Cancer Inst. 1978 Mar;60(3):649-52. doi: 10.1093/jnci/60.3.649.

Abstract

Maytansine is a new drug undergoing clinical investigation. It has functional similarities to vincristine. Maytansine and vincristine were given to CDF1 mice with P388 leukemic ascites, and the cytokinetic response of the tumor cells was analyzed with a flow microfluorometer; mithramycin was used as the DNA fluorochrome. The results indicated a similar series of cytokinetic effects after administration of both drugs, though these effects were greater and more persistent after maytansine was given. Although both drugs produced some degree of multinucleation and endoreduplication, vincristine produced a discrete population of cells with a DNA content (fluorescence) equivalent to octoploidy (8C). Microscopy of the sorted 8C cells at 24 hours indicated 54% multinucleation and 33% mitotic figures. Most cells remained blocked in the G1-phase for at least 96 hours after administration of both drugs, which indicated that rapid DNA content distributions can be used to determine not only the effects of drugs on cell cycle distribution but also the duration of drug action.

摘要

美登素是一种正在进行临床研究的新药。它与长春新碱在功能上有相似之处。将美登素和长春新碱给予患有P388白血病腹水的CDF1小鼠,并使用流式微荧光计分析肿瘤细胞的细胞动力学反应;光辉霉素用作DNA荧光染料。结果表明,两种药物给药后有一系列相似的细胞动力学效应,不过给予美登素后的这些效应更强烈且更持久。虽然两种药物都产生了一定程度的多核化和核内再复制,但长春新碱产生了一群DNA含量(荧光)相当于八倍体(8C)的离散细胞群体。对分选的8C细胞在24小时时进行显微镜检查,结果显示54%为多核化,33%为有丝分裂图像。给予两种药物后,大多数细胞至少在G1期停滞96小时,这表明快速的DNA含量分布不仅可用于确定药物对细胞周期分布的影响,还可用于确定药物作用的持续时间。

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