Automated large-scale AMD progression prediction using machine-read OCT biomarkers

Author:

Rudas AkosORCID,Chiang Jeffrey N.,Corradetti GiuliaORCID,Rakocz Nadav,Halperin Eran,Sadda Srinivas R.ORCID

Abstract

AbstractAge-related Macular Degeneration (AMD) is a major cause of irreversible vision loss in individuals over 55 years old in the United States. While anti-vascular growth factor injections can be used to treat macular neovascularization (MNV), there are currently no treatments available to halt or reverse geographic atrophy, which is the late-stage of nonneovascular AMD. There is a great interest in detecting early biomarkers associated with a higher risk for AMD progression in order to design early intervention clinical trials. The annotation of structural biomarkers on optical coherence tomography (OCT) B-scans is a laborious, complex and time-consuming process, and discrepancies between human graders can introduce variability into this assessment.To address this issue, a deep-learning model (SLIVER-net) was proposed, which could identify AMD biomarkers on structural OCT volumes with high precision and without human supervision. However, the validation was performed on a small dataset, and the true predictive power of these detected biomarkers in the context of a large cohort has not been evaluated. In this retrospective cohort study, we perform the largest-scale validation of these biomarkers to date. We also assess how these features combined with other EHR data (demographics, comorbidities, etc) affect and/or improve the prediction performance relative to known factors. Our hypothesis is that these biomarkers can be identified by a machine learning algorithm without human supervision, in a way that they preserve their predictive nature.The way we test this hypothesis is by building several machine learning models utilizing these machine-read biomarkers, and assessing their added predictive power. We found that not only can we show that the machine-read OCT B-scan biomarkers are predictive of AMD progression, we also observe that our proposed combined OCT and EHR data-based algorithm significantly outperforms the state-of-the-art solution in clinically relevant metrics and provides actionable information which has the potential to improve patient care. In addition, it provides a framework for automated large-scale processing of OCT volumes, making it possible to analyze vast archives without human supervision.

Publisher

Cold Spring Harbor Laboratory

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