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1-β-D-阿拉伯呋喃糖基胞嘧啶、胸腺嘧啶核苷和羟基脲在体外对人B细胞和白血病原始细胞的协同相互作用。

Synergistic interaction between 1-beta-D-arabinofuranosylcytosine, thymidine, and hydroxyurea against human B cells and leukemic blasts in vitro.

作者信息

Streifel J A, Howell S B

出版信息

Proc Natl Acad Sci U S A. 1981 Aug;78(8):5132-6. doi: 10.1073/pnas.78.8.5132.

Abstract

Isobologram analysis was used to examine the interaction between 1-beta-D-arabinofuranosylcytosine (Ara-C), thymidine (dThd), and hydroxyurea. All three pairs of drugs, as well as the triple combination, were synergistic against a human B cell line in vitro across a broad range of concentrations. Synergy was associated with an increase in the Ara-C nucleotide pool and Ara-C triphosphate concentration. dThd increased, and hydroxyurea decreased, the incorporation of Ara-C into trichloroacetic acid-insoluble macromolecules per unit time. Hydroxyurea was more effective than dThd at equimolar concentrations in increasing the acid-soluble Ara-C pool. Maximal stimulation of Ara-C triphosphate formation by dThd occurred at 1 mM and was associated with reduction of the deoxycytidine triphosphate pool to 31% of control. At the same concentration, hydroxyurea increased Ara-C triphosphate formation to a greater extent but increased deoxycytidine triphosphate to 116% of control. When tested at clinically achievable concentrations on blasts from patients with acute leukemia, hydroxyurea increased the Ara-C nucleotide pool in all six cases studied, whereas dThd decreased the Ara-C nucleotide pool. These results indicate that in SB cells dThd and hydroxyurea work by different mechanisms to augment the Ara-C nucleotide pool and that hydroxyurea may be more effective than dThd as a modulator of Ara-C activity in patients with acute leukemia.

摘要

采用等效线图分析来检测1-β-D-阿拉伯呋喃糖基胞嘧啶(阿糖胞苷,Ara-C)、胸腺嘧啶核苷(dThd)和羟基脲之间的相互作用。在广泛的浓度范围内,所有三对药物组合以及三联组合在体外对人B细胞系均具有协同作用。协同作用与阿糖胞苷核苷酸池和阿糖胞苷三磷酸浓度的增加有关。dThd增加而羟基脲减少单位时间内阿糖胞苷掺入三氯乙酸不溶性大分子中的量。在等摩尔浓度下,羟基脲比dThd在增加酸溶性阿糖胞苷池方面更有效。dThd对阿糖胞苷三磷酸形成的最大刺激作用发生在1 mM,且与脱氧胞苷三磷酸池减少至对照的31%相关。在相同浓度下,羟基脲在更大程度上增加了阿糖胞苷三磷酸的形成,但使脱氧胞苷三磷酸增加至对照的116%。当在急性白血病患者的原始细胞上以临床可达到的浓度进行测试时,羟基脲在所研究的所有6例病例中均增加了阿糖胞苷核苷酸池,而dThd则减少了阿糖胞苷核苷酸池。这些结果表明,在SB细胞中,dThd和羟基脲通过不同机制增加阿糖胞苷核苷酸池,并且在急性白血病患者中,羟基脲作为阿糖胞苷活性调节剂可能比dThd更有效。

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