• Cancer Chemother. Pharmacol. · Aug 2009

    The xc- cystine/glutamate antiporter as a potential therapeutic target for small-cell lung cancer: use of sulfasalazine.

    • Jun Guan, Maisie Lo, Peter Dockery, Sarah Mahon, Cristina M Karp, Arthur R Buckley, Stephen Lam, Peter W Gout, and Yu-Zhuo Wang.
    • Department of Cancer Endocrinology, BC Cancer Agency, Research Centre, Vancouver, BC, Canada.
    • Cancer Chemother. Pharmacol. 2009 Aug 1;64(3):463-72.

    PurposeTo determine whether the xc- cystine transporter could be a useful therapeutic target for small-cell lung cancer (SCLC).MethodsHuman SCLC cell cultures were examined for growth dependence on extracellular cystine, xc- expression, glutathione levels and response to highly specific xc- inhibitors, i.e., monosodium glutamate (MSG) and the anti-inflammatory drug, sulfasalazine (SASP). In studying tumor growth inhibition by SASP, use was also made of a novel SCLC tissue xenograft model, LU6-SCLC, derived from a chemoresistant patient's SCLC specimen.ResultsGrowth of NCI-H69 and NCI-H82 SCLC cells greatly depended on xc- -mediated uptake of cystine. SASP substantially reduced their glutathione levels (>70%; 0.3 mM SASP; 24 h) and growth (72 h) with IC(50)s of 0.21 and 0.13 mM, respectively; MSG also inhibited growth markedly. Both SASP- and MSG-induced growth arrests were largely prevented by cystine uptake-enhancing 2-mercaptoethanol (66 approximately microM) indicating they were primarily due to cystine starvation. Without major side-effects, SASP (i.p.) restrained growth of NCI-H69 cell xenografts (approximately 50%) and, importantly, substantially inhibited growth of the clinically more relevant LU6-SCLC tissue xenografts (approximately 70% by stereological analysis), reducing tumor glutathione contents.ConclusionsThe xc- cystine/glutamate antiporter is potentially useful as a target for therapy of SCLC based on glutathione depletion. Sulfasalazine may be readily used for this approach, especially in combination chemotherapy.

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