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. 2017 Jul 1;19(7):908-917.
doi: 10.1093/neuonc/now312.

Leveraging molecular datasets for biomarker-based clinical trial design in glioblastoma

Shyam K Tanguturi  1 Lorenzo Trippa  1 Shakti H Ramkissoon  1 Kristine Pelton  1 David Knoff  1 David Sandak  1 Neal I Lindeman  1 Azra H Ligon  1 Rameen Beroukhim  1 Giovanni Parmigiani  1 Patrick Y Wen  1 Keith L Ligon  1 Brian M Alexander  1
Affiliations

Leveraging molecular datasets for biomarker-based clinical trial design in glioblastoma

Shyam K Tanguturi et al. Neuro Oncol. .

Abstract

Background: Biomarkers can improve clinical trial efficiency, but designing and interpreting biomarker-driven trials require knowledge of relationships among biomarkers, clinical covariates, and endpoints. We investigated these relationships across genomic subgroups of glioblastoma (GBM) within our institution (DF/BWCC), validated results in The Cancer Genome Atlas (TCGA), and demonstrated potential impacts on clinical trial design and interpretation.

Methods: We identified genotyped patients at DF/BWCC, and clinical associations across 4 common GBM genomic biomarker groups were compared along with overall survival (OS), progression-free survival (PFS), and survival post-progression (SPP). Significant associations were validated in TCGA. Biomarker-based clinical trials were simulated using various assumptions.

Results: Epidermal growth factor receptor (EGFR)(+) and p53(-) subgroups were more likely isocitrate dehydrogenase (IDH) wild-type. Phosphatidylinositol-3 kinase (PI3K)(+) patients were older, and patients with O6-DNA methylguanine-methyltransferase (MGMT)-promoter methylation were more often female. OS, PFS, and SPP were all longer for IDH mutant and MGMT methylated patients, but there was no independent prognostic value for other genomic subgroups. PI3K(+) patients had shorter PFS among IDH wild-type tumors, however, and no DF/BWCC long-term survivors were either EGFR(+) (0% vs 7%, P = .014) or p53(-) (0% vs 10%, P = .005). The degree of biomarker overlap impacted the efficiency of Bayesian-adaptive clinical trials, while PFS and OS distribution variation had less impact. Biomarker frequency was proportionally associated with sample size in all designs.

Conclusions: We identified several associations between GBM genomic subgroups and clinical or molecular prognostic covariates and validated known prognostic factors in all survival periods. These results are important for biomarker-based trial design and interpretation of biomarker-only and nonrandomized trials.

Keywords: biomarkers; clinical trial design; glioblastoma.

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Figures

Fig. 1
Fig. 1
Biomarker status by individual in the DF/BWCC cohorts and TCGA cohorts. Status of IDH, MGMT, EGFR, PI3K, p53, and CDK biomarker groups for each individual patient are arranged in columns in both the DF/BWCC and TCGA cohorts. Trial-eligible GBM patients include those without IDH mutation or 1p/19q codeletion.
Fig. 2
Fig. 2
Hazard ratios for OS, PFS, and SPP by biomarker subgroups in TCGA and DF/BWCC patient cohorts. *Outcomes across IDH subgroups were compared across the entire cohort. Outcomes across remaining biomarker subgroups were compared across only trial-eligible GBM-patients (IDH WT). Hazard ratios are displayed for positive biomarker status relative to negative status as the baseline, with HR <1 representing a favorable endpoint. Point estimates for the HR are displayed by a square box, scaled to the representative sample size of biomarker (+) patients, with 95% CIs displayed in horizontal bars.
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