SDZ PSC-833, A NONIMMUNOSUPPRESSIVE CYCLOSPORINE - ITS POTENCY IN OVERCOMING P-GLYCOPROTEIN-MEDIATED MULTIDRUG RESISTANCE OF MURINE LEUKEMIA

被引：109

作者：

KELLER, RP

ALTERMATT, HJ

NOOTER, K

POSCHMANN, G

LAISSUE, JA

BOLLINGER, P

HIESTAND, PC

机构：

[1] SANDOZ PHARMA LTD,PRECLIN RES,CH-4056 BASEL,SWITZERLAND

[2] UNIV BERN,INST PATHOL,CH-3010 BERN,SWITZERLAND

[3] TNO,INST APPL RADIOBIOL & IMMUNOL,2288 GJ RIJSWIJK,NETHERLANDS

来源：

INTERNATIONAL JOURNAL OF CANCER | 1992年 / 50卷 / 04期

关键词：

D O I：

10.1002/ijc.2910500418

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Cyclosporin A (CsA, Sandimmune) is known to reverse P-glycoprotein(P-gp170)-mediated multidrug resistance as efficiently as other prototype compounds of resistance modifiers. The immunosuppressive activity and nephrotoxicity of CsA, however, may limit its clinical use. PSC-833, a new cyclosporine, exerts a similar resistance-modifying activity but lacks toxicity or immunosuppressive activity. We have tested its potency in vitro and in vivo on the L1210 leukemia cell line transfected with a full-length cDNA copy of the human mdrI gene, which showed a stable 30-fold resistance towards adriamycin as compared to the parental cell line. In vitro growth of the transfected cell was unchanged. In vivo growth was less aggressive; the survival time of inoculated mice was prolonged. In vitro, PSC-833 was at least as potent as CsA or verapamil in reversing multidrug resistance. In vivo, the drug-resistant L1210 leukemia was completely unresponsive to i.v. monotherapy with adriamycin at its maximum tolerated dose (MTD). PSC-833 enhanced the activity and toxicity of adriamycin. The MTD of adriamycin was about 3 times lower than when given alone. On this basis, the MTD of i.v. adriamycin in combination with oral PSC-833 successfully overcame refractoriness to treatment. Survival times of the mice were considerably prolonged and even some cures of leukemic mice occurred.

引用

页码：593 / 597

页数：5

共 29 条

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