Linking stress-signaling,glutathione metabolism,signaling pathways and xenobiotic transporters |
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Authors: | Sushma Yadav Ewa Zajac Sharad S. Singhal Sanjay Awasthi |
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Affiliation: | (1) Department of Chemistry and Biochemistry, University of Texas at Arlington, 700 Planetarium Place, CPB Room # 312, Arlington, TX 76019-0065, USA |
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Abstract: | Multi-specific drug-transport mechanisms are intricately involved in mediating a pleiotropic drug-resistance in cancer cells by mediating drug-accumulation defects in cells in which they are over-expressed. The existence and over-expression in drug-resistant neoplasms of transporter proteins belonging to ATP-binding cassette (ABC) family indicate that these myriad transporters contribute to the multidrug-resistance phenomena by removing or sequestering of toxins and metabolites. Another prominent mechanism of multispecific drug-resistance involves glutathione and glutathione linked enzymes, particularly those of the mercapturic acid pathway, which are involved in metabolism and excretion of both endogenous and exogenous electrophilic toxins. A key step in the mercapturic acid pathway, efflux of the glutathione-electrophile conjugate has recently been shown to be catalyzed largely by the stress-responsive protein RLIP76, a splice variant peptide endowed by the human gene RALBP1. The known involvement of RLIP76 in membrane signaling pathways and endocytosis has resulted in a new paradigm for transport and metabolism related drug-resistance in which RLIP76 plays a central role. Our recent studies demonstrating a key anti-apoptotic and stress-responsive role of RLIP76, and the demonstration of dramatic response in malignancies to RLIP76 depletion indicate that targeting this mercapturic acid pathway transporter may be a highly effective and multifaceted antineoplastic strategy. |
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Keywords: | Glutathione Oxidative stress RLIP76 4-hydroxynonenal Drug resistance Signaling ABC transporters Doxorubicin siRNA Non-ABC transporters |
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