[No authors listed]
AIMS:This study uncovered that the genetically endowed intracellular glutathione contents (iGSH) regulated by the catalytic subunit of γâglutamylcysteine synthetase heavy chain (γâGCSh) as a prime target for overcoming both the inherited and stimuli-activated chemo- and radio-resistance of hepatocellular carcinoma (HCC) cells. MAIN METHODS:Reactive oxygen species production and mitochondrial membrane potential (ÎÏm) were determined by the probe-based flow cytometry. The TUNEL assay was used as an index of radio-sensitivity and the MTT assay was used as an index of chemo-sensitivity against various anti-cancer agents. iGSH and γâGCSh activity were measured by HPLC methods. γâGCSh-overexpressing GCS30 cell line was established by tetracycline-controlled Tet-OFF gene expression system in SK-Hep-1 cells. KEY FINDINGS:The relative radio-sensitivities of a panel of five HCC cells were found to be correlated negatively with both the contents of iGSH and their corresponding γâGCSh activities with an order of abundance being Hep G2â¯>â¯Hep 3Bâ¯>â¯J5â¯>â¯Mahlavuâ¯>â¯SK-Hep-1, respectively. Similarly, the cytotoxicity response patterns of these HCC cells against arsenic trioxide (ATO), a anti-cancer drug, were exactly identical to the order of ranking instigated by the radiotherapy (RT) treatment. Next, γâGCSh-overexpressing GCS30 cells were found to possess excellent ability to profoundly mitigate both the drop of ÎÏm and apoptotic TUNEL-positive cell population engendered by ATO, cisplatin, doxorubicin, and RT treatments. SIGNIFICANCE:Our data unequivocally demonstrate that γâGCSh may represent a prime target for overcoming anti-cancer drugs and RT resistance for HCC cells.
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