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British journal of cancer · Mar 2015
Observational StudyIL8 polymorphisms and overall survival in pazopanib- or sunitinib-treated patients with renal cell carcinoma.
- C-F Xu, T Johnson, J Garcia-Donas, T K Choueiri, C N Sternberg, I D Davis, N Bing, K C Deen, Z Xue, L McCann, E Esteban, J C Whittaker, C F Spraggs, C Rodríguez-Antona, L N Pandite, and R J Motzer.
- GlaxoSmithKline, Gunnels Wood Road, Stevenage SG1 2NY, UK.
- Br. J. Cancer. 2015 Mar 31; 112 (7): 1190-8.
BackgroundWe evaluated germline single nucleotide polymorphisms (SNPs) for association with overall survival (OS) in pazopanib- or sunitinib-treated patients with advanced renal cell carcinoma (aRCC).MethodsThe discovery analysis tested 27 SNPs within 13 genes from a phase III pazopanib trial (N=241, study 1). Suggestive associations were then pursued in two independent datasets: a phase III trial (COMPARZ) comparing pazopanib vs sunitinib (N=729, study 2) and an observational study of sunitinib-treated patients (N=89, study 3).ResultsIn study 1, four SNPs showed nominally significant association (P≤0.05) with OS; two of these SNPs (rs1126647, rs4073) in IL8 were associated (P≤0.05) with OS in study 2. Because rs1126647 and rs4073 were highly correlated, only rs1126647 was evaluated in study 3, which also showed association (P≤0.05). In the combined data, rs1126647 was associated with OS after conservative multiple-test adjustment (P=8.8 × 10(-5); variant vs reference allele hazard ratio 1.32, 95% confidence interval: 1.15-1.52), without evidence for heterogeneity of effects between studies or between pazopanib- and sunitinib-treated patients.ConclusionsVariant alleles of IL8 polymorphisms are associated with poorer survival outcomes in pazopanib- or sunitinib-treated patients with aRCC. These findings provide insight in aRCC prognosis and may advance our thinking in development of new therapies.
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