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抗肿瘤蒽环类药物对人白血病细胞生长抑制的生化参数

Biochemical parameters of growth inhibition of human leukemia cells by antitumor anthracycline agents.

作者信息

Schwartz H S, Kanter P M

出版信息

Cancer Treat Rep. 1979 May;63(5):821-5.

PMID:287555
Abstract

Ten antitumor anthracycline derivatives used in this study inhibit growth of a human leukemia cell line over a range of potencies exceeding four orders of magnitude. The agents vary from each other at C-4 and C-13, with stereochemical differences at C-4' and substitutions at C-14 and N. Drug retention, DNA damage, and inhibition of DNA synthesia are parameters used to express potency of the agents in a mathematic model. Estimates of DNA damage are sufficient, however, to describe growth inhibition by a single agent (4-demethoxydaunorubicin). It may be possible now to attempt to extend the model to predict therapeutic responses to a number of anthracyclines, thereby enhancing the clinical utility of this important class of agents.

摘要

本研究中使用的10种抗肿瘤蒽环类衍生物在超过四个数量级的效力范围内抑制人白血病细胞系的生长。这些药物在C-4和C-13处彼此不同,在C-4'处存在立体化学差异,在C-14和N处有取代基。药物滞留、DNA损伤和DNA合成抑制是用于在数学模型中表达药物效力的参数。然而,DNA损伤的估计足以描述单一药物(4-去甲氧基柔红霉素)对生长的抑制作用。现在或许有可能尝试扩展该模型以预测对多种蒽环类药物的治疗反应,从而提高这类重要药物的临床效用。

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