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Current Oncology is published by MDPI from Volume 28 Issue 1 (2021). Previous articles were published by another publisher in Open Access under a CC-BY (or CC-BY-NC-ND) licence, and they are hosted by MDPI on mdpi.com as a courtesy and upon agreement with Multimed Inc..
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Article

V体育ios版 - Potential Use of the Anti-Inflammatory Drug, Sulfasalazine, for Targeted Therapy of Pancreatic Cancer

1
Department of Cancer Genetics, BC Cancer Agency, and Department of Experimental Medicine, University of British Columbia, Vancouver, BC, Canada
2
Department of Cancer Endocrinology, BC Cancer Agency, Vancouver, BC, Canada
3
The Prostate Centre, Vancouver General Hospital, and Department of Urologic Sciences, University of British Columbia, Vancouver, BC, Canada
*
Author to whom correspondence should be addressed. (V体育2025版)
Curr. Oncol. 2010, 17(3), 9-16; https://doi.org/10.3747/co.v17i3.485
Submission received: 1 May 2010 / Revised: 4 May 2010 / Accepted: 14 May 2010 / Published: 1 June 2010

"VSports注册入口" Abstract

Pancreatic cancer is an aggressive, drug-resistant disease; its first-line chemotherapeutic, gemcitabine, is only marginally effective. Intracellular depletion of glutathione, a major free-radical scavenger, has been associated with growth arrest and reduced drug resistance (chemosensitization) of cancer cells. In search of a new therapeutic approach for pancreatic cancer, we sought to determine whether specific inhibition of the plasma membrane xc− cystine transporter could lead to reduced uptake of cysteine, a key precursor of glutathione, and subsequent glutathione depletion. Sulfasalazine (approximately 0.2 mmol/L), an anti-inflammatory drug with potent xc−-inhibitory properties, markedly reduced L-[14C]-cystine uptake, glutathione levels, and growth and viability of human MIA PaCa-2 and PANC-1 pancreatic cancer cells in vitro. These effects were shown to result primarily from inhibition of cystine uptake mediated by the xc− cystine transporter and not from inhibition of nuclear factor κB activation, another property of sulfasalazine. The efficacy of gemcitabine could be markedly enhanced by combination therapy with sulfasalazine both in vitro and in immunodeficient mice carrying xenografts of the same cell lines. No major side effects were observed in vivo. The results of the present study suggest that the xc – transporter plays a major role in pancreatic cancer by sustaining or enhancing glutathione biosynthesis, and as such, represents a potential therapeutic target. Sulfasalazine, a relatively nontoxic drug approved by the U.S. Food and Drug Administration, may, in combination with gemcitabine, lead to more effective therapy of refractory pancreatic cancer.
Keywords: pancreatic cancer; xc−cystine transporter; sulfasalazine; cystine; cysteine; glutathione; gemcitabine resistance; NFKB pancreatic cancer; xc−cystine transporter; sulfasalazine; cystine; cysteine; glutathione; gemcitabine resistance; NFKB

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MDPI and ACS Style

Lo, M. ; Ling, V. ; Low, C. ; Wang, Y. Z. ; Gout, P. W. Potential Use of the Anti-Inflammatory Drug, Sulfasalazine, for Targeted Therapy of Pancreatic Cancer. Curr V体育官网入口. Oncol. 2010, 17, 9-16. https://doi. org/10. 3747/co. v17i3. 485 .

AMA Style

Lo M, Ling V, Low C, Wang YZ, Gout PW. Potential Use of the Anti-Inflammatory Drug, Sulfasalazine, for Targeted Therapy of Pancreatic Cancer. Current Oncology. 2010; 17(3):9-16. https://doi.org/10.3747/co.v17i3.485

Chicago/Turabian Style

Lo, M., V. Ling, C. Low, Y.Z. Wang, and P.W. Gout. 2010. "Potential Use of the Anti-Inflammatory Drug, Sulfasalazine, for Targeted Therapy of Pancreatic Cancer" Current Oncology 17, no. 3: 9-16. https://doi.org/10.3747/co.v17i3.485

APA Style

Lo, M., Ling, V., Low, C., Wang, Y. Z., & Gout, P. W. (2010). Potential Use of the Anti-Inflammatory Drug, Sulfasalazine, for Targeted Therapy of Pancreatic Cancer. Current Oncology, 17(3), 9-16. https://doi.org/10.3747/co.v17i3.485

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