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Effects of ouabain on NIH/3T3 cells transformed with retrovirai oncogenes and on human tumor cell lines

✍ Scribed by Pierosandro Tagliaferri; Kazuyoshi Yanagihara; Fortunate Ciardiello; Neil Talbot; Ursula Flatow; Leonard Benade; Robert H. Bassin

Publisher: John Wiley and Sons
Year: 1987
Tongue: French
Weight: 596 KB
Volume: 40
Category: Article
ISSN: 0020-7136
DOI: 10.1002/ijc.2910400514

No coin nor oath required. For personal study only.

✦ Synopsis

Both murine and human cell lines transformed by the v-Kiras gene have been shown to be much more sensitive to the toxic effects of the cardiac glycoside ouabain than their respective controls. This differential toxicity has previously been used in the isolation of flat revertant clones from populations of Kirsten murine sarcoma virus transformed NIH/3T3 cells. Here, we have undertaken a further characterization of this phenomenon in murine and human tumor cells. Two different techniques, a "Cr-release assay and a quantitative Crystal violet elution assay, have been employed to compare the sensitivities to ouabain of normal and v-Ki-raptransformed NIH/3T3 cells. In each assay, ras-transformed NIH13T3 cell lines displayed an increased sensitivity to ouabain as compared to the parental NIH13T3 cell line, both in dose-response and in time-course experiments. In a separate study, ouabain was also able to inhibit the growth in semi-solid medium of 2 v-Ki-ra+transformed NIH/3T3 cell lines (DT and K-NIH) in a dose-dependent fashion. The same concentrations of ouabain were effective in both the "Cr-release and Crystal violet assays. To address the question of whether increased sensitivity to ouabain is a specific result of transformation with the ras oncogene or is a common event which accompanies transformation by other oncogenes, we have screened a variety of transformed NIH/3T3 derivatives. All of these lines displayed an increased sensitivity to ouabain when compared to the parental NIH/3T3 cell line. ' To whom reprint requests should be addressed at NCI Bldg.

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