Literature DB >> 2803945

Role of the aclacinomycin A--doxorubicin association in reversal of doxorubicin resistance in K562 tumour cells.

J M Millot1, T D Rasoanaivo, H Morjani, M Manfait.   

Abstract

Acquired resistance to anthracyclines is characterised by a lower sensitivity to these agents, associated with impaired accumulation of drug. We have examined the ability of aclacinomycin A (ACM) associated with doxorubicin (DOX), to increase intranuclear DOX concentrations and, consequently, to enhance cytotoxic effects against drug resistant cells in vitro. A recently developed microspectrofluorometric technique is used to measure intranuclear DOX concentrations in sensitive and DOX-resistant K562 cells treated with DOX and ACM. Fluorescence emission spectra are collected from a microvolume of single living cell nuclei. From both DOX and ACM model fluorescence spectra (free, DNA-bound and metabolites), the intranuclear spectral profile is analysed according to the amount of each component. This quantitative analysis determines intranuclear DOX concentrations with an error of 10%. Non-cytotoxic doses of ACM, in combination with DOX, increase cytotoxic activity of DOX against K562 resistant cells. When DOX-resistant cells are exposed simultaneously to ACM and DOX, significant increases in intranuclear DOX concentrations are found compared with the case of exposure to DOX alone. The measure of the intranuclear retention of DOX shows that ACM partly blocks the DOX efflux in resistant cell nuclei, resulting in enhanced accumulation of DOX. These data lead us to conclude that ACM-DOX association partly reverses the DOX resistance at clinically achievable concentrations.

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Year:  1989        PMID: 2803945      PMCID: PMC2247305          DOI: 10.1038/bjc.1989.339

Source DB:  PubMed          Journal:  Br J Cancer        ISSN: 0007-0920            Impact factor:   7.640


  32 in total

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2.  Correlation between growth inhibition and intranuclear doxorubicin and 4'-deoxy-4'-iododoxorubicin quantitated in living K562 cells by microspectrofluorometry.

Authors:  M Gigli; T W Rasoanaivo; J M Millot; P Jeannesson; V Rizzo; J C Jardillier; F Arcamone; M Manfait
Journal:  Cancer Res       Date:  1989-02-01       Impact factor: 12.701

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Authors:  M Manfait; A J Alix; P Jeannesson; J C Jardillier; T Theophanides
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4.  Exploitable mechanisms in combined radiotherapy-chemotherapy: the concept of additivity.

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5.  Combination chemotherapy with a new anthracycline glycoside, aclacinomycin-A, and active drugs for malignant lymphomas in P388 mouse leukemia system.

Authors:  S Fujimoto; J Inagaki; N Horikoshi; M Ogawa
Journal:  Gan       Date:  1979-08

6.  NADPH cytochrome P-450 reductase activation of quinone anticancer agents to free radicals.

Authors:  N R Bachur; S L Gordon; M V Gee; H Kon
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7.  Plasma kinetics of aclacinomycin A and its major metabolites in man.

Authors:  M J Egorin; D Van Echo; B M Fox; M Whitacre; N R Bachur
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8.  The interaction of daunorubicin and doxorubicin with DNA and chromatin.

Authors:  F Zunino; A Di Marco; A Zaccara; R A Gambetta
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9.  High performance liquid chromatographic determination of aclacinomycin a and its related compounds. II. Reverse phase HPLC determination of aclacinomycin A and its metabolites in biological fluids using fluorescence detection.

Authors:  T Ogasawara; Y Masuda; S Goto; S Mori; T Oki
Journal:  J Antibiot (Tokyo)       Date:  1981-01       Impact factor: 2.649

10.  Comparative nuclear and cellular incorporation of daunorubicin, doxorubicin, carminomycin, marcellomycin, aclacinomycin A and AD 32 in daunorubicin-sensitive and -resistant Ehrlich ascites in vitro.

Authors:  S Seeber; H Loth; S T Crooke
Journal:  J Cancer Res Clin Oncol       Date:  1980       Impact factor: 4.553

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3.  Human hepatoma cells rich in P-glycoprotein are sensitive to aclarubicin and resistant to three other anthracyclines.

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