Data from Development and Multicenter Case–Control Validation of Urinary Comprehensive Genomic Profiling for Urothelial Carcinoma Diagnosis, Surveillance, and Risk-Prediction

Jason J Lee,Brian C Mazzarella,Martha E Evans-Holm,Andrew Pienkny,Mahdi Goudarzi,Trevor G Levin,Vincent M Caruso,Vincent T Bicocca,Yair Lotan,Debasish Sundi,Chi K Lee,Peter S Lentz,Gabrielle Difiore,Monica Garcia-Ransom,Greg Barme,Adam S Feldman,Joel Piser,Iden J Haddadzadeh,Daniel S Fischer,Andrew R Macbride,Theresa M Koppie,Kevin G Phillips,Joe W Gray,Shulin Wu,Keyan Salari,Edward J Collins ,Daniel T Oberlin ,Robert L Kahn ,Qiuxia Yan ,Chin-Lee Wu

doi:10.1158/1078-0432.c.6779668

Abstract

<div>AbstractPurpose:<p>Urinary comprehensive genomic profiling (uCGP) uses next-generation sequencing to identify mutations associated with urothelial carcinoma and has the potential to improve patient outcomes by noninvasively diagnosing disease, predicting grade and stage, and estimating recurrence risk.</p>Experimental Design:<p>This is a multicenter case–control study using banked urine specimens collected from patients undergoing initial diagnosis/hematuria workup or urothelial carcinoma surveillance. A total of 581 samples were analyzed by uCGP: 333 for disease classification and grading algorithm development, and 248 for blinded validation. uCGP testing was done using the UroAmp platform, which identifies five classes of mutation: single-nucleotide variants, copy-number variants, small insertion-deletions, copy-neutral loss of heterozygosity, and aneuploidy. UroAmp algorithms predicting urothelial carcinoma tumor presence, grade, and recurrence risk were compared with cytology, cystoscopy, and pathology.</p>Results:<p>uCGP algorithms had a validation sensitivity/specificity of 95%/90% for initial cancer diagnosis in patients with hematuria and demonstrated a negative predictive value (NPV) of 99%. A positive diagnostic likelihood ratio (DLR) of 9.2 and a negative DLR of 0.05 demonstrate the ability to risk-stratify patients presenting with hematuria. In surveillance patients, binary urothelial carcinoma classification demonstrated an NPV of 91%. uCGP recurrence-risk prediction significantly prognosticated future recurrence (hazard ratio, 6.2), whereas clinical risk factors did not. uCGP demonstrated positive predictive value (PPV) comparable with cytology (45% vs. 42%) with much higher sensitivity (79% vs. 25%). Finally, molecular grade predictions had a PPV of 88% and a specificity of 95%.</p>Conclusions:<p>uCGP enables noninvasive, accurate urothelial carcinoma diagnosis and risk stratification in both hematuria and urothelial carcinoma surveillance patients.</p></div>

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