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Development and Validation of a Novel Integrated Clinical-Genomic Risk Group Classification for Localized Prostate Cancer
- Spratt, Daniel E;
- Zhang, Jingbin;
- Santiago-Jiménez, María;
- Dess, Robert T;
- Davis, John W;
- Den, Robert B;
- Dicker, Adam P;
- Kane, Christopher J;
- Pollack, Alan;
- Stoyanova, Radka;
- Abdollah, Firas;
- Ross, Ashley E;
- Cole, Adam;
- Uchio, Edward;
- Randall, Josh M;
- Nguyen, Hao;
- Zhao, Shuang G;
- Mehra, Rohit;
- Glass, Andrew G;
- Lam, Lucia LC;
- Chelliserry, Jijumon;
- du Plessis, Marguerite;
- Choeurng, Voleak;
- Aranes, Maria;
- Kolisnik, Tyler;
- Margrave, Jennifer;
- Alter, Jason;
- Jordan, Jennifer;
- Buerki, Christine;
- Yousefi, Kasra;
- Haddad, Zaid;
- Davicioni, Elai;
- Trabulsi, Edouard J;
- Loeb, Stacy;
- Tewari, Ashutosh;
- Carroll, Peter R;
- Weinmann, Sheila;
- Schaeffer, Edward M;
- Klein, Eric A;
- Karnes, R Jeffrey;
- Feng, Felix Y;
- Nguyen, Paul L
- et al.
Published Web Location
https://doi.org/10.1200/jco.2017.74.2940Abstract
Purpose It is clinically challenging to integrate genomic-classifier results that report a numeric risk of recurrence into treatment recommendations for localized prostate cancer, which are founded in the framework of risk groups. We aimed to develop a novel clinical-genomic risk grouping system that can readily be incorporated into treatment guidelines for localized prostate cancer. Materials and Methods Two multicenter cohorts (n = 991) were used for training and validation of the clinical-genomic risk groups, and two additional cohorts (n = 5,937) were used for reclassification analyses. Competing risks analysis was used to estimate the risk of distant metastasis. Time-dependent c-indices were constructed to compare clinicopathologic risk models with the clinical-genomic risk groups. Results With a median follow-up of 8 years for patients in the training cohort, 10-year distant metastasis rates for National Comprehensive Cancer Network (NCCN) low, favorable-intermediate, unfavorable-intermediate, and high-risk were 7.3%, 9.2%, 38.0%, and 39.5%, respectively. In contrast, the three-tier clinical-genomic risk groups had 10-year distant metastasis rates of 3.5%, 29.4%, and 54.6%, for low-, intermediate-, and high-risk, respectively, which were consistent in the validation cohort (0%, 25.9%, and 55.2%, respectively). C-indices for the clinical-genomic risk grouping system (0.84; 95% CI, 0.61 to 0.93) were improved over NCCN (0.73; 95% CI, 0.60 to 0.86) and Cancer of the Prostate Risk Assessment (0.74; 95% CI, 0.65 to 0.84), and 30% of patients using NCCN low/intermediate/high would be reclassified by the new three-tier system and 67% of patients would be reclassified from NCCN six-tier (very-low- to very-high-risk) by the new six-tier system. Conclusion A commercially available genomic classifier in combination with standard clinicopathologic variables can generate a simple-to-use clinical-genomic risk grouping that more accurately identifies patients at low, intermediate, and high risk for metastasis and can be easily incorporated into current guidelines to better risk-stratify patients.
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