Your search keyword '"Peter S. Lentz"' showing total 3 results

1. Urinary comprehensive genomic profiling predicts urothelial carcinoma recurrence and identifies responders to intravesical therapy

Author

Goran Rac, Hiten D. Patel, Christopher James, Shalin Desai, Vincent M. Caruso, Daniel S. Fischer, Peter S. Lentz, Ceressa T. Ward, Brian C. Mazzarella, Kevin G. Phillips, Chirag Doshi, Vincent T. Bicocca, Trevor G. Levin, Alan J. Wolfe, and Gopal N. Gupta

Subjects

Bacillus Calmette‐Guérin, bladder cancer, genomics, intravesical instillation, personalized medicine, risk assessment, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Intravesical therapy (IVT) is the standard of care to decrease risk of recurrence and progression for high‐grade nonmuscle‐invasive bladder cancer. However, post‐IVT recurrence remains common and the ability to risk‐stratify patients before or after IVT is limited. In this prospectively designed and accrued cohort study, we examine the utility of urinary comprehensive genomic profiling (uCGP) for predicting recurrence risk following transurethral resection of bladder tumor (TURBT) and evaluating longitudinal IVT response. Urine was collected before and after IVT instillation and uCGP testing was done using the UroAmp™ platform. Baseline uCGP following TURBT identified patients with high (61%) and low (39%) recurrence risk. At 24 months, recurrence‐free survival (RFS) was 100% for low‐risk and 45% for high‐risk patients with a hazard ratio (HR) of 9.3. Longitudinal uCGP classified patients as minimal residual disease (MRD) Negative, IVT Responder, or IVT Refractory with 24‐month RFS of 100%, 50%, and 32%, respectively. Compared with MRD Negative patients, IVT Refractory patients had a HR of 10.5. Collectively, uCGP enables noninvasive risk assessment of patients following TURBT and induction IVT. uCGP could inform surveillance cystoscopy schedules and identify high‐risk patients in need of additional therapy.

Published

2024

2. MP22-19 URINARY COMPREHENSIVE GENOMIC PROFILING PREDICTS UROTHELIAL CANCER UP TO 12 YEARS AHEAD OF CLINICAL DIAGNOSIS. AN EXPANDED ANALYSIS OF THE GOLESTAN COHORT STUDY

Author

Yair Lotan, Keyan Salari, Adam Feldman, Debasish Sundi, Jason J Lee, Gabrielle DiFiore, Hossein Poustchi, Masoud Khoshnia, Gholamreza Roshandel, Arash Etemadi, Mahdi Goudarzi, Peter S. Lentz, Kevin G. Phillips, Vincent T. Bicocca, Theresa M. Koppie, Joe W. Gray, Trevor Levin, Reza Malekzadeh, Mahdi Sheikh, and Florence Le Calvez-Kelm

Subjects

Urology

Published

2023

3. Urinary Comprehensive Genomic Profiling Correlates Urothelial Carcinoma Mutations with Clinical Risk and Efficacy of Intervention

Author

Vincent T. Bicocca, Kevin G. Phillips, Daniel S. Fischer, Vincent M. Caruso, Mahdi Goudarzi, Monica Garcia-Ransom, Peter S. Lentz, Andrew R. MacBride, Brad W. Jensen, Brian C. Mazzarella, Theresa Koppie, James E. Korkola, Joe W. Gray, and Trevor G. Levin

Subjects

General Medicine, bladder cancer, next generation sequencing, machine learning, genomic profiling, liquid biopsy, urine

Abstract

The clinical standard of care for urothelial carcinoma (UC) relies on invasive procedures with suboptimal performance. To enhance UC treatment, we developed a urinary comprehensive genomic profiling (uCGP) test, UroAmplitude, that measures mutations from tumor DNA present in urine. In this study, we performed a blinded, prospective validation of technical sensitivity and positive predictive value (PPV) using reference standards, and found at 1% allele frequency, mutation detection performs at 97.4% sensitivity and 80.4% PPV. We then prospectively compared the mutation profiles of urine-extracted DNA to those of matched tumor tissue to validate clinical performance. Here, we found tumor single-nucleotide variants were observed in the urine with a median concordance of 91.7% and uCGP revealed distinct patterns of genomic lesions enriched in low- and high-grade disease. Finally, we retrospectively explored longitudinal case studies to quantify residual disease following bladder-sparing treatments, and found uCGP detected residual disease in patients receiving bladder-sparing treatment and predicted recurrence and disease progression. These findings demonstrate the potential of the UroAmplitude platform to reliably identify and track mutations associated with UC at each stage of disease: diagnosis, treatment, and surveillance. Multiple case studies demonstrate utility for patient risk classification to guide both surgical and therapeutic interventions.

Published

2022