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D-维拉帕米下调P170相关的对阿霉素、柔红霉素和伊达比星的耐药性。

D-verapamil downmodulates P170-associated resistance to doxorubicin, daunorubicin and idarubicin.

作者信息

Damiani D, Michieli M, Michelutti A, Melli C, Cerno M, Baccarani M

机构信息

Chair of Anatomy, Udine University School of Medicine, Italy.

出版信息

Anticancer Drugs. 1993 Apr;4(2):173-80. doi: 10.1097/00001813-199304000-00007.

Abstract

Verapamil (VRP) is an effective modulator of P170-associated multidrug resistance (MDR), but its clinical application is limited by cardiovascular side-effects. The D-isomer of VRP (D-VRP) is 10 times less active than the racemic mixture on the cardiovascular system, but retains a MDR modulating activity. Daunorubicin (DNR) and doxorubicin (DX) are two anthracyclines whose cytotoxicity is strongly related with the expression of P170, while their respective lipophylic derivatives idarubicin (IDA) and iododoxorubicin (IDX) are less P170-dependent. We studied the effect of D-VRP on intracellular retention and on the cytotoxicity of these four anthracyclines in two MDR cell systems (LOVO and CEM) by flow cytometry and by a microcultured tetrazolium colorimetric assay (MTT). We found that in MDR cells D-VRP increased intracellular anthracycline concentration and increased the cytotoxicity of DNR, IDA and DX but not of IDX. The effect of D-VRP was dose-related, but it was already consistent at D-VRP concentrations that can be readily maintained in vivo (2-3 microM). These data suggest that at a clinically tolerable concentration D-VRP can downmodulate the resistance to DNR and DX and can restore full sensitivity to IDA.

摘要

维拉帕米(VRP)是P170相关多药耐药(MDR)的有效调节剂,但其临床应用受到心血管副作用的限制。VRP的D-异构体(D-VRP)在心血管系统上的活性比消旋混合物低10倍,但保留了MDR调节活性。柔红霉素(DNR)和阿霉素(DX)是两种蒽环类药物,其细胞毒性与P170的表达密切相关,而它们各自的亲脂性衍生物伊达比星(IDA)和碘阿霉素(IDX)对P170的依赖性较小。我们通过流式细胞术和微量培养四唑盐比色法(MTT)研究了D-VRP对两种MDR细胞系(LOVO和CEM)中这四种蒽环类药物的细胞内滞留和细胞毒性的影响。我们发现,在MDR细胞中,D-VRP增加了细胞内蒽环类药物的浓度,并增加了DNR、IDA和DX的细胞毒性,但未增加IDX的细胞毒性。D-VRP的作用与剂量相关,但在体内易于维持的D-VRP浓度(2-3 microM)下就已经很明显。这些数据表明,在临床可耐受浓度下,D-VRP可以下调对DNR和DX的耐药性,并可以恢复对IDA的完全敏感性。

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