| Autor: |
Alam, Ridwan, Aguirre, Aaron, Stultz, Collin |
| Rok vydání: |
2023 |
| Předmět: |
|
| Druh dokumentu: |
Working Paper |
| DOI: |
10.1371/journal.pdig.0000539 |
| Popis: |
For a number of antiarrhythmics, drug loading requires a 3 day hospitalization with monitoring for QT prolongation. Automated QT monitoring with wearable ECG monitors would facilitate out-of-hospital care. We develop a deep learning model that infers QT intervals from ECG lead-I - the lead most often acquired from ambulatory ECG monitors - and to use this model to detect clinically meaningful QT-prolongation episodes during Dofetilide drug loading. Using 4.22 million 12-lead ECG recordings from 903.6 thousand patients at the Massachusetts General Hospital, we develop a deep learning model, QTNet, that infers QT intervals from lead-I. Over 3 million ECGs from 653 thousand patients are used to train the model and an internal-test set containing 633 thousand ECGs from 135 thousand patients was used for testing. QTNet is further evaluated on an external-validation set containing 3.1 million ECGs from 667 thousand patients at another institution. QTNet was used to detect Dofetilide-induced QT prolongation in a publicly available database (ECGRDVQ-dataset) containing ECGs from subjects enrolled in a clinical trial evaluating the effects of antiarrhythmic drugs. QTNet achieves mean absolute errors of 12.63ms (internal-test) and 12.30ms (external-validation) for estimating absolute QT intervals. The associated Pearson correlation coefficients are 0.91 (internal-test) and 0.92 (external-validation). For the ECGRDVQ-dataset, QTNet detects Dofetilide-induced QTc prolongation with 87% sensitivity and 77% specificity. The negative predictive value of the model is greater than 95% when the pre-test probability of drug-induced QTc prolongation is below 25%. Drug-induced QT prolongation risk can be tracked from ECG lead-I using deep learning. |
| Databáze: |
arXiv |
| Externí odkaz: |
|
