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ICRF-187(右丙亚胺)对细胞中蒽环类半醌形成的抑制作用。

Inhibition of anthracycline semiquinone formation by ICRF-187 (dexrazoxane) in cells.

作者信息

Malisza K L, Hasinoff B B

机构信息

Faculty of Pharmacy, University of Manitoba, Winnipeg, Canada.

出版信息

Free Radic Biol Med. 1996;20(7):905-14. doi: 10.1016/0891-5849(95)02188-4.

Abstract

The formation of semiquinone free radicals of doxorubicin, epirubicin, daunorubicin, and idarubicin was measured by electron paramagnetic resonance (EPR) spectroscopy in hypoxic suspensions of chinese hamster ovary (CHO) cells. The amount of semiquinone produced was in the order idarubicin >> doxorubicin > daunorubicin > epirubicin. The idarubicin semiquinone signal was both the fastest to be formed and to decay. Idarubicin, which was the most lipophilic of the anthracyclines studied, also displayed the fastest fluorescence-measured cellular uptake of drug. Thus, it was concluded that semiquinone formation was dependent upon the rate of cellular uptake. Lysed cell suspensions were also shown to be capable of producing the doxorubicin semiquinone in the presence of added NADPH. The cardioprotective agent dexrazoxane (ICRF-187) was observed to decrease the amount of doxorubicin semiquinone observed in cell suspensions. Dexrazoxane also decreased the amount of doxorubicin semiquinone observed in the NADPH-lysed cell suspension mixture. Neither bipyridine nor deferoxamine decreased NADPH-dependent doxorubicin semiquinone formation. These results suggest that dexrazoxane does not decrease doxorubicin semiquinone formation through an iron complex formed from hydrolyzed dexrazoxane. Dexrazoxane may be inhibiting an NADPH-dependent enzyme.

摘要

通过电子顺磁共振(EPR)光谱法,在中国仓鼠卵巢(CHO)细胞的缺氧悬浮液中测量了阿霉素、表柔比星、柔红霉素和伊达比星半醌自由基的形成。产生的半醌量顺序为伊达比星>>阿霉素>柔红霉素>表柔比星。伊达比星半醌信号形成和衰减最快。在所研究的蒽环类药物中,伊达比星的亲脂性最强,其通过荧光测量的细胞对药物的摄取也最快。因此,得出结论,半醌的形成取决于细胞摄取速率。还显示在添加NADPH的情况下,裂解的细胞悬浮液能够产生阿霉素半醌。观察到心脏保护剂右丙亚胺(ICRF - 187)可减少细胞悬浮液中观察到的阿霉素半醌量。右丙亚胺还减少了在NADPH裂解的细胞悬浮液混合物中观察到的阿霉素半醌量。联吡啶和去铁胺均未减少NADPH依赖性阿霉素半醌的形成。这些结果表明,右丙亚胺并非通过水解右丙亚胺形成的铁络合物来减少阿霉素半醌的形成。右丙亚胺可能是在抑制一种NADPH依赖性酶。

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