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The Radiogenomic Risk Score: Construction of a Prognostic Quantitative, Noninvasive Image-based Molecular Assay for Renal Cell Carcinoma

Purpose:
To evaluate the feasibility of constructing radiogenomic-based surrogates of molecular assays (SOMAs) in patients with clear-cell renal cell carcinoma (CCRCC) by using data extracted from a single computed tomographic (CT) image.

Materials and Methods:
In this institutional review board approved study, gene expression profile data and contrast material–enhanced CT images from 70 patients with CCRCC in a training set were independently assessed by two radiologists for a set of predefined imaging features. A SOMA for a previously validated CCRCC-specific supervised principal component (SPC) risk score prognostic gene signature was construct-ed and termed the radiogenomic risk score (RRS). It uses the microarray data and a 28-trait image array to evaluate each CT image with multiple regression of gene expres-sion analysis. The predictive power of the RRS SOMA was then prospectively validated in an independent dataset to confirm its relationship to the SPC gene signature (n = 70) and determination of patient outcome (n = 77). Data were analyzed by using multivariate linear regression–based methods and Cox regression modeling, and significance was assessed with receiver operator characteristic curves and Kaplan-Meier survival analysis.

Results:
Our SOMA faithfully represents the tissue-based molec-ular assay it models. The RRS scaled with the SPC gene signature (R = 0.57, P , .001, classification accuracy 70.1%, P , .001) and predicted disease-specific survival (log rank P , .001). Independent validation confirmed the relationship between the RRS and the SPC gene signa-ture (R = 0.45, P , .001, classification accuracy 68.6%, P , .001) and disease-specific survival (log-rank P , .001) and that it was independent of stage, grade, and performance status (multivariate Cox model P , .05, log-rank P , .001).

Conclusion:
A SOMA for the CCRCC-specific SPC prognostic gene sig-nature that is predictive of disease-specific survival and independent of stage was constructed and validated, con-firming that SOMA construction is feasible.

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Jamshidi N., Jonasch E., Zapala M., Korn R.L., Aganovic L., Zhao H., Tumkur Sitaram R., Tibshirani R.J., Banerjee S., Brooks J.D., Ljungberg B. and Kuo MD. “The Radiogenomic Risk Score: Construction of a Prognostic Quantitative, Noninvasive Image-based Molecular Assay for Renal Cell Carcinoma.” Radiology, 277(1): 114-23, (2015).

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