Accelerated Metabolism and Exclusion of 4-Hydroxynonenal through Induction of RLIP76 and hGST5.8 Is an Early Adaptive Response of Cells to Heat and Oxidative Stress

Jizhong Cheng; Rajendra Sharma; Yusong Yang; Sharad S. Singhal; Abha Sharma; Manjit K. Saini; Shivendra V. Singh; Piotr Zimniak; Sanjay Awasthi; Sanjay Awasthi

doi:10.1074/jbc.m106838200

Accelerated Metabolism and Exclusion of 4-Hydroxynonenal through Induction of RLIP76 and hGST5.8 Is an Early Adaptive Response of Cells to Heat and Oxidative Stress

Jizhong Cheng(The University of Texas Medical Branch at Galveston), Rajendra Sharma(The University of Texas Medical Branch at Galveston), Yusong Yang(The University of Texas Medical Branch at Galveston), Sharad S. Singhal(The University of Texas at Arlington), Abha Sharma(The University of Texas Medical Branch at Galveston), Manjit K. Saini(The University of Texas Medical Branch at Galveston), Shivendra V. Singh(UPMC Hillman Cancer Center), Piotr Zimniak(Central Arkansas Veterans Healthcare System), Sanjay Awasthi(The University of Texas at Arlington), Sanjay Awasthi(The University of Texas Medical Branch at Galveston)

Journal of Biological Chemistry

November 1, 2001

10.1074/jbc.m106838200

Cited by 185Open Access

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Abstract

To explore the role of lipid peroxidation (LPO) products in the initial phase of stress mediated signaling, we studied the effect of mild, transient oxidative or heat stress on parameters that regulate the cellular concentration of 4-hydroxynonenal (4-HNE). When K562 cells were exposed to mild heat shock (42 °C, 30 min) or oxidative stress (50 µmH2O2, 20 min) and allowed to recover for 2 h, there was a severalfold induction of hGST5.8, which catalyzes the formation of glutathione-4-HNE conjugate (GS-HNE), and RLIP76, which mediates the transport of GS-HNE from cells (Awasthi, S., Cheng, J., Singhal, S. S., Saini, M. K., Pandya, U., Pikula, S., Bandorowicz-Pikula, J., Singh, S. V., Zimniak, P., and Awasthi, Y. C. (2000) Biochemistry 39, 9327–9334). Enhanced LPO was observed in stressed cells, but the major antioxidant enzymes and HSP70 remained unaffected. The stressed cells showed higher GS-HNE-conjugating activity and increased efflux of GS-HNE. Stress-pre-conditioned cells with induced hGST5.8 and RLIP76 acquired resistance to 4-HNE and H2O2-mediated apoptosis by suppressing a sustained activation of c-Jun N-terminal kinase and caspase 3. The protective effect of stress pre-conditioning against apoptosis was abrogated by coating the cells with anti-RLIP76 IgG, which inhibited the efflux of GS-HNE from cells, indicating that the cells acquired resistance to apoptosis by metabolizing and excluding 4-HNE at a higher rate. Induction of hGST5.8 and RLIP76 by mild, transient stress and the resulting resistance of stress-pre-conditioned cells to apoptosis appears to be a general phenomenon since it was not limited to K562 cells but was also evident in lung cancer cells, H-69, H-226, human leukemia cells, HL-60, and human retinal pigmented epithelial cells. These results strongly suggest a role of LPO products, particularly 4-HNE, in the initial phase of stress mediated signaling.

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