Development and Validation of a Deep Learning Algorithm for Gleason Grading of Prostate Cancer From Biopsy Specimens

Development and Validation of a Deep Learning Algorithm for Gleason Grading of Prostate Cancer From Biopsy Specimens

For prostate cancer, Gleason grading of the biopsy specimen plays a pivotal role in determining case management. However, Gleason grading is associated with substantial interobserver variability, resulting in a need for decision support tools to improve the reproducibility of Gleason grading in rout...

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Bibliographic Details
Published in:JAMA oncology Vol. 6; no. 9; p. 1372
Main Authors: Nagpal, Kunal, Foote, Davis, Tan, Fraser, Liu, Yun, Chen, Po-Hsuan Cameron, Steiner, David F, Manoj, Naren, Olson, Niels, Smith, Jenny L, Mohtashamian, Arash, Peterson, Brandon, Amin, Mahul B, Evans, Andrew J, Sweet, Joan W, Cheung, Carol, van der Kwast, Theodorus, Sangoi, Ankur R, Zhou, Ming, Allan, Robert, Humphrey, Peter A, Hipp, Jason D, Gadepalli, Krishna, Corrado, Greg S, Peng, Lily H, Stumpe, Martin C, Mermel, Craig H
Format: Journal Article
Language:English
Published: United States 01-09-2020
Subjects:
Adolescent
Adult
Algorithms
Artificial Intelligence
Biopsy, Large-Core Needle - methods
Deep Learning
Humans
Image Interpretation, Computer-Assisted
Male
Neoplasm Grading - standards
Prostatic Neoplasms - diagnosis
Prostatic Neoplasms - epidemiology
Prostatic Neoplasms - pathology
Specimen Handling
United States - epidemiology
Young Adult
United States
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Summary:For prostate cancer, Gleason grading of the biopsy specimen plays a pivotal role in determining case management. However, Gleason grading is associated with substantial interobserver variability, resulting in a need for decision support tools to improve the reproducibility of Gleason grading in routine clinical practice. To evaluate the ability of a deep learning system (DLS) to grade diagnostic prostate biopsy specimens. The DLS was evaluated using 752 deidentified digitized images of formalin-fixed paraffin-embedded prostate needle core biopsy specimens obtained from 3 institutions in the United States, including 1 institution not used for DLS development. To obtain the Gleason grade group (GG), each specimen was first reviewed by 2 expert urologic subspecialists from a multi-institutional panel of 6 individuals (years of experience: mean, 25 years; range, 18-34 years). A third subspecialist reviewed discordant cases to arrive at a majority opinion. To reduce diagnostic uncertainty, all subspecialists had access to an immunohistochemical-stained section and 3 histologic sections for every biopsied specimen. Their review was conducted from December 2018 to June 2019. The frequency of the exact agreement of the DLS with the majority opinion of the subspecialists in categorizing each tumor-containing specimen as 1 of 5 categories: nontumor, GG1, GG2, GG3, or GG4-5. For comparison, the rate of agreement of 19 general pathologists' opinions with the subspecialists' majority opinions was also evaluated. For grading tumor-containing biopsy specimens in the validation set (n = 498), the rate of agreement with subspecialists was significantly higher for the DLS (71.7%; 95% CI, 67.9%-75.3%) than for general pathologists (58.0%; 95% CI, 54.5%-61.4%) (P < .001). In subanalyses of biopsy specimens from an external validation set (n = 322), the Gleason grading performance of the DLS remained similar. For distinguishing nontumor from tumor-containing biopsy specimens (n = 752), the rate of agreement with subspecialists was 94.3% (95% CI, 92.4%-95.9%) for the DLS and similar at 94.7% (95% CI, 92.8%-96.3%) for general pathologists (P = .58). In this study, the DLS showed higher proficiency than general pathologists at Gleason grading prostate needle core biopsy specimens and generalized to an independent institution. Future research is necessary to evaluate the potential utility of using the DLS as a decision support tool in clinical workflows and to improve the quality of prostate cancer grading for therapy decisions.
ISSN:2374-2445
DOI:10.1001/jamaoncol.2020.2485