Induction of Heat-Shock Protein Synthesis and Thermotolerance in EL-4 Ascites Tumor Cells by Transient ATP Depletion after Ischemic Stress

The effect of a short-term energy deprivation (ischemia) on thermoresistance and heat-shock protein (HSP) synthesis in murine ascites EL-4 thymoma cells was studied in vitro. The incubation of the cells in glucose-free medium with rotenone (respiratory inhibitor) for 10 min caused rapid ATP depletio...

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Published inExperimental and molecular pathology Vol. 60; no. 2; pp. 88 - 99
Main Authors Gabai, Vladimir L., Kabakov, Alexander E.
Format Journal Article
LanguageEnglish
Russian
Published Amsterdam Elsevier Inc 01.04.1994
Elsevier
Subjects
2,4-Dinitrophenol
Adenosine Triphosphate - metabolism
Adenosine Triphosphate - physiology
Animals
Dinitrophenols - pharmacology
Energy Metabolism
Heat-Shock Proteins - metabolism
Hot Temperature
Hydrogen-Ion Concentration
In Vitro Techniques
Ischemia - metabolism
Ischemia - physiopathology
Mice
Mice, Inbred C57BL
Oxygen - physiology
Rotenone - pharmacology
Thymoma - metabolism
Thymoma - pathology
Thymus Neoplasms - metabolism
Thymus Neoplasms - pathology
Time Factors
Tumor Cells, Cultured
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Summary:The effect of a short-term energy deprivation (ischemia) on thermoresistance and heat-shock protein (HSP) synthesis in murine ascites EL-4 thymoma cells was studied in vitro. The incubation of the cells in glucose-free medium with rotenone (respiratory inhibitor) for 10 min caused rapid ATP depletion (to 9% of the initial level). After recovery, the synthesis of HSP70 and HSP90 was stimulated in the cells and they became greatly more resistant to hyperthermia than the control cells. The simultaneous rotenone and thermal treatment significantly decreased cell viability. The transition of HSP70 to Triton X-100-insoluble cell fraction was found in the ATP-depleted cells as well as in the heat-shocked cells, and 1 m M ATP fully reversed such insolubilization when it was added in Triton extraction buffer. The data obtained reveal that transient ATP depletion per se is sufficient to result in the HSP70 insolubilization, thus being conducive to induction of HSP synthesis and thermotolerance in the cells which recovered after energy deprivation. A novel mechanism of protein aggregation in ATP-deficient cells and a possible role of transient ischemia in development of tumor thermotolerance in vivo are discussed.
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ISSN:0014-4800
1096-0945
DOI:10.1006/exmp.1994.1008