The PCR products were then sequenced on an ABI Prism 3130xl Genetic Analyzer (Applied Biosystems) as per the instructions from the manufacturer. Statistical considerations The progression free or overall survival based on genotype or toxicity groups (grade ≥ 2/grade < 2) was estimated by the Kaplan-Meier method [16] and compared by the exact log-rank test. Deviation from Hardy-Weinberg equilibrium was tested separately for different ethnic groups, using the Chi-squared test. The impact of genotypes selleck compound on treatment-associated toxicities
and the association between toxicities were assessed by Fisher’s exact test. All statistical analyses were two-tailed at a pre-specified significance level of < 0.05. In view of the exploratory nature of analysis, P-values were not formally corrected for multiple testing. SAS for Windows version 9.1.3 was used for these statistical analyses. Results Genotyping data The genotype and allele frequencies of studied VEGFR2 SNPs are shown in Table 2. Both VEGFR2 SNPs were in Hardy-Weinberg equilibrium (P ≥ 0.77) when evaluated in Caucasian patients (n = 140) and African American patients (n = 17). Hardy-Weinberg equilibrium was not assessed in Hispanics and Asians (n = 13). There was no linkage between the two VEGFR2 SNPs (P > 0.05) in any of the studied populations. Table 2 Genotype and allele frequencies for SNP in VEGFR2 loci for patients treated with
sorafenib and/or bevacizumab, with or without other agents Allelic learn more variant N Genotype frequencies, N (%) Allelic frequencies Wt Het Var p q VEGFR2 H472Q 170 C* 140 82 50 8 0.76 0.24 AA* 17 12 5 0 0.85 0.15 Others 13 9 4 0 N/A N/A VEGFR2 V297I 170 C* 140 114 25 1 0.9 0.1 AA* 17 9 6 2 0.71 0.29 Others 13 8 5 0 N/A N/A * Genotyping information was not available for n = 7 Caucasians and n = 1 African American included in subsequent analyses. C: Caucasians, AA: African-Americans, Others: Hispanic or Asians, Wt: wild-type genotype, Het: heterozygous genotype, Var: homozygous variant genotype, p and q are standard Hardy-Weinberg nomenclature for allele frequencies. HT and HFSR as phenotypic Adenosine triphosphate markers for PFS and OS Because drug-induced
toxicities may be directly related to the 4SC-202 activity of bevacizumab and sorafenib, we hypothesized that these toxicities may also predict the progression free survival (PFS) and overall survival (OS) following anti-VEGF therapy. Patients on BAY-KS were not included in the survival analysis since this cohort was small with limited survival data. When the other 5 clinical trials presented in Table 1 were examined individually, we determined that HT was associated with prolonged PFS in patients treated with bevacizumab on the APC-CRPC and BAY-BEV trials (P = 0.0009, and P = 0.052 respectively). The median PFS difference was 14.9 (HT < grade 2, n = 45) versus 31.5 months (HT ≥ grade 2, n = 15) in patients participating on the APC-CRPC trial (Figure 1A), and 3.