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Multi‐Institutional Phase II Study of S‐1 Monotherapy in Advanced Gastric Cancer with Pharmacokinetic and Pharmacogenomic Evaluations

This study describes the first phase II study of S‐1, a novel oral fluoropyrimidine, in a non‐Japanese Asian population with advanced gastric cancer. S‐1 was administered twice daily for 28 days every 6 weeks. A pharmacokinetic study was performed on day 28 of cycles 1 and 3. Genomic DNA from periph...

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Published in:The oncologist (Dayton, Ohio) Ohio), 2007-05, Vol.12 (5), p.543-554
Main Authors: Jeung, Hei‐Cheul, Rha, Sun Young, Kim, Hoon Kyo, Lim, Ho Young, Kim, Samyong, Kim, Si Young, Gong, Soo Jeong, Park, Chan Hee, Ahn, Joong Bae, Noh, Sung Hoon, Chung, Hyun Cheol
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Language:English
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Summary:This study describes the first phase II study of S‐1, a novel oral fluoropyrimidine, in a non‐Japanese Asian population with advanced gastric cancer. S‐1 was administered twice daily for 28 days every 6 weeks. A pharmacokinetic study was performed on day 28 of cycles 1 and 3. Genomic DNA from peripheral mononuclear cells was analyzed using a cDNA microarray‐based comparative genomic hybridization (CGH) method. Thirty‐one patients were initially given a dose of 35 mg/m2 twice daily (bid) (group 1); then, the protocol was amended by increasing the dose to 40 mg/m2 bid for an additional 31 patients (group 2) because of good tolerability to S‐1. The overall response rate was 19.3% (95% confidence interval, 9.2%–29.5%). Over a median follow‐up duration of 265 days, the median time to progression and overall survival time were 126 and 264 days, respectively. The 1‐year survival rate was 34%. There was no grade 4 toxicity and the major adverse event was anemia. Pharmacokinetic parameters were similar to those of the previous Japanese reports. Microarray CGH identified 18 genes with copy number changes that were associated with hemoglobin reduction with S‐1 treatment. A logistic regression analysis, integrating one clinical parameter (initial hemoglobin level) combined with three genetic copy number variations (HIST1H2BL, C10orf127, and XPNPEP2), provided a predictive model for the development of severe hemoglobin reduction. In conclusion, this study showed the feasibility of using S‐1 at 35 mg/m2 bid in gastric cancer. We suggest that the pharmacogenomic markers identified in this study may be potential candidates for predicting anemia after S‐1 treatment. Disclosure of potential conflicts of interest is found at the end of this article.
ISSN:1083-7159
1549-490X
DOI:10.1634/theoncologist.12-5-543