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Cross-resistance pattern of cell lines selected for resistance towards different cytotoxic drugs to membrane-toxic phospholipids in vitro.

Authors :
Himmelmann, Andreas
Danhauser-Riedl, Susanne
Steinhauser, Gabriela
Busch, Raymonde
Modest, Edward
Noseda, Alessandro
Rastetter, Johann
Ralph Vogler, W.
Berdel, Wolfgang
Himmelmann, A W
Danhauser-Riedl, S
Steinhauser, G
Busch, R
Modest, E J
Noseda, A
Rastetter, J
Vogler, W R
Berdel, W E
Source :
Cancer Chemotherapy & Pharmacology; Sep1990, Vol. 26 Issue 6, p437-443, 7p
Publication Year :
1990

Abstract

The synthetic ether lipids ET-18-OCH3 and BM41.440 and a derivative, hexadecylphosphocholine, were tested for inhibition of [3H]-thymidine uptake into a Chinese hamster ovarian cell line (AUXBl) and its multidrug-resistant subline selected for colchicine resistance (CHRC5). The activity of all three compounds against the multidrug-resistant subline was equal to or higher than that against the parent line. The same result was found for their activity against a human leukemic lymphoblastic cell line (CEM/O) and its methotrexate-resistant subline (CEM/MTX). In contrast, two multidrug-resistant cell lines selected for resistance to Adriamycin, the mouse leukemia cell line P388/ADR and the murine sarcoma cell line S180/ADR, expressed modest cross-resistance to the lipids as measured by thymidine uptake. Experiments performed using the trypan-blue dye-exclusion assay yielded comparable results, although this system revealed a slightly different sensitivity in showing the cytotoxicity of the drugs. By this assay, modest cross-resistance for ET-18-OCH3 and BM41.440 to Adriamycin was found only after 24 h incubation and decreased after 48 h incubation, with almost equal sensitivity to both drugs being shown by the parental (P388/W) and resistant lines (P388/ADR). Furthermore, findings from a human tumor-cloning assay were in accordance with these data, although they did not indicate cross-resistance for the P388/ADR cell line. These results suggest that certain ether lipids and derivatives might represent valuable anticancer drugs warranting further study in the setting of resistant disease. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
03445704
Volume :
26
Issue :
6
Database :
Complementary Index
Journal :
Cancer Chemotherapy & Pharmacology
Publication Type :
Academic Journal
Accession number :
71001124
Full Text :
https://doi.org/10.1007/BF02994095