Abstract
BackgroundCurrent risk models for renal cell carcinoma (RCC) based on clinicopathological factors are sub-optimal in accurately identifying high-risk patients. Here, we perform a head-to-head comparison of previously published DNA methylation markers and propose a potential prognostic model for clear cell RCC (ccRCC).Patients and methodsPromoter methylation of PCDH8, BNC1, SCUBE3, GREM1, LAD1, NEFH, RASSF1A, GATA5, SFRP1, CDO1, and NEURL was determined by nested methylation-specific PCR. To identify clinically relevant methylated regions, The Cancer Genome Atlas (TCGA) was used to guide primer design. Formalin-fixed paraffin-embedded (FFPE) tissue samples from 336 non-metastatic ccRCC patients from the prospective Netherlands Cohort Study (NLCS) were used to develop a Cox proportional hazards model using stepwise backward elimination and bootstrapping to correct for optimism. For validation purposes, FFPE ccRCC tissue of 64 patients from the University Hospitals Leuven and a series of 232 cases from The Cancer Genome Atlas (TCGA) were used.ResultsMethylation of GREM1, GATA5, LAD1, NEFH, NEURL, and SFRP1 was associated with poor ccRCC-specific survival, independent of age, sex, tumor size, TNM stage or tumor grade. Moreover, the association between GREM1, NEFH, and NEURL methylation and outcome was shown to be dependent on the genomic region. A prognostic biomarker model containing GREM1, GATA5, LAD1, NEFH and NEURL methylation in combination with clinicopathological characteristics, performed better compared to the model with clinicopathological characteristics only (clinical model), in both the NLCS and the validation population with a c-statistic of 0.71 versus 0.65 and a c-statistic of 0.95 versus 0.86 consecutively. However, the biomarker model had limited added prognostic value in the TCGA series with a c-statistic of 0.76 versus 0.75 for the clinical model.ConclusionIn this study we performed a head-to-head comparison of potential prognostic methylation markers for ccRCC using a novel approach to guide primers design which utilizes the optimal location for measuring DNA methylation. Using this approach, we identified five methylation markers that potentially show prognostic value in addition to currently known clinicopathological factors.
Highlights
Renal cell carcinoma (RCC) is the most common malignant neoplasm of the kidney and accounts for 2–3% of the total human cancer burden [1]
Methylation of GREM1, GATA5, LAD1, NEFH, NEURL, and SFRP1 was associated with poor clear cell RCC (ccRCC)-specific survival, independent of age, sex, tumor size, TNM stage or tumor grade
In this study we performed a head-to-head comparison of potential prognostic methylation markers for ccRCC using a novel approach to guide primers design which utilizes the optimal location for measuring DNA meth‐ ylation
Summary
Renal cell carcinoma (RCC) is the most common malignant neoplasm of the kidney and accounts for 2–3% of the total human cancer burden [1]. Despite the fact that current clinical characteristics or prognostic models, such as the TNM staging system, Fuhrman grading, the Stage, Size, Grade, and Necrosis (SSIGN) Risk Score, and the University of California Los Angeles Integrated Staging System (UISS), are considered to be strong prognostic indicators [4,5,6,7], these do not yet lead to the desired accuracy in predicting patient outcome. There is a need to identify and develop additional molecular prognostic markers that can enhance the predictive performance of current prognostic models [5, 9,10,11,12,13]. Current risk models for renal cell carcinoma (RCC) based on clinicopathological factors are sub-optimal in accurately identifying high-risk patients. We perform a head-to-head comparison of previously published DNA methylation markers and propose a potential prognostic model for clear cell RCC (ccRCC)
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