Inhibition of Cystine Uptake Disrupts the Growth of Primary Brain Tumors

Glial cells play an important role in sequestering neuronally released glutamate via Na+-dependent transporters. Surprisingly, these transporters are not operational in glial-derived tumors (gliomas). Instead, gliomas release glutamate, causing excitotoxic death of neurons in the vicinity of the tum...

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Bibliographic Details
Published in:The Journal of neuroscience 2005-08, Vol.25 (31), p.7101-7110
Main Authors: Chung, Wook Joon, Lyons, Susan A, Nelson, Gina M, Hamza, Hashir, Gladson, Candece L, Gillespie, G. Yancey, Sontheimer, Harald
Format: Article
Language:English
Subjects:
Amino Acid Transport Systems - antagonists & inhibitors
Amino Acid Transport Systems - metabolism
Animals
Apoptosis
Benzoates - pharmacology
Brain Neoplasms - metabolism
Brain Neoplasms - pathology
Brain Neoplasms - physiopathology
Caspases - metabolism
Cell Division - drug effects
Cystine - antagonists & inhibitors
DNA, Neoplasm - antagonists & inhibitors
Glutathione - antagonists & inhibitors
Glycine - analogs & derivatives
Glycine - pharmacology
Humans
Neurobiology of Disease
Rats
Rats, Sprague-Dawley
Sulfasalazine - pharmacology
Time Factors
Tumor Cells, Cultured
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Summary:Glial cells play an important role in sequestering neuronally released glutamate via Na+-dependent transporters. Surprisingly, these transporters are not operational in glial-derived tumors (gliomas). Instead, gliomas release glutamate, causing excitotoxic death of neurons in the vicinity of the tumor. We now show that glutamate release from glioma cells is an obligatory by-product of cellular cystine uptake via system xc-, an electroneutral cystine-glutamate exchanger. Cystine is an essential precursor for the biosynthesis of glutathione, a major redox regulatory molecule that protects cells from endogenously produced reactive oxygen species (ROS). Glioma cells, but not neurons or astrocytes, rely primarily on cystine uptake via system xc- for their glutathione synthesis. Inhibition of system xc- causes a rapid depletion of glutathione, and the resulting loss of ROS defense causes caspase-mediated apoptosis. Glioma cells can be rescued if glutathione status is experimentally restored or if glutathione is substituted by alternate cellular antioxidants, confirming that ROS are indeed mediators of cell death. We describe two potent drugs that permit pharmacological inhibition of system xc-. One of these drugs, sulfasalazine, is clinically used to treat inflammatory bowel disease and rheumatoid arthritis. Sulfasalazine was able to reduce glutathione levels in tumor tissue and slow tumor growth in vivo in a commonly used intracranial xenograft animal model for human gliomas when administered by intraperitoneal injection. These data suggest that inhibition of cystine uptake into glioma cells through the pharmacological inhibition of system xc- may be a viable therapeutic strategy with a Food and Drug Administration-approved drug already in hand.
ISSN:0270-6474
1529-2401
DOI:10.1523/JNEUROSCI.5258-04.2005