Deep Radiomics Detection of Clinically Significant Prostate Cancer on Multicenter MRI: Initial Comparison to PI-RADS Assessment

Objective: To develop and evaluate a deep radiomics model for clinically significant prostate cancer (csPCa, grade group>= 2) detection and compare its performance to Prostate Imaging Reporting and Data System (PI-RADS) assessment in a multicenter cohort. Materials and Methods: This retrospective study analyzed biparametric (T2W and DW) prostate MRI sequences of 615 patients (mean age, 63.1 +/- 7 years) from four datasets acquired between 2010 and 2020: PROSTATEx challenge, Prostate158 challenge, PCaMAP trial, and an in-house (NTNU/St. Olavs Hospital) dataset. With expert annotations as ground truth, a deep radiomics model was trained, including nnU-Net segmentation of the prostate gland, voxel-wise radiomic feature extraction, extreme gradient boost classification, and post-processing of tumor probability maps into csPCa detection maps. Training involved 5-fold cross-validation using the PROSTATEx (n=199), Prostate158 (n=138), and PCaMAP (n=78) datasets, and testing on the in-house (n=200) dataset. Patient- and lesion-level performance were compared to PI-RADS using area under ROC curve (AUROC [95% CI]), sensitivity, and specificity analysis. Results: On the test data, the radiologist achieved a patient-level AUROC of 0.94 [0.91-0.98] with 94% (75/80) sensitivity and 77% (92/120) specificity at PI-RADS>= 3. The deep radiomics model at a tumor probability cut-off>= 0.76 achieved 0.91 [0.86-0.95] AUROC with 90% (72/80) sensitivity and 73% (87/120) specificity, not significantly different (p = 0.068) from PI-RADS. On the lesion level, PI-RADS cut-off>= 3 had 84% (91/108) sensitivity at 0.2 (40/200) false positives per patient, while deep radiomics attained 68% (73/108) sensitivity at the same false positive rate. Conclusion: Deep radiomics machine learning model achieved comparable performance to PI-RADS assessment in csPCa detection at the patient-level but not at the lesion-level.