Database Open Access
ECG Effects of Ranolazine, Dofetilide, Verapamil, and Quinidine
Published: July 26, 2016. Version: 1.0.0
New Database Added: ECGRDVQ (July 26, 2016, midnight)
The ECG Effects of Ranolazine, Dofetilide, Verapamil, and Quinidine in Healthy Subjects database contains multi-channel ECG recordings of subjects partaking in a randomized, double-blind, 5-period crossover clinical trial aimed at comparing the effects of four known QT prolonging drugs versus placebo on electrophysiological and other clinical parameters.
Please include the standard citation for PhysioNet:
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Goldberger, A., Amaral, L., Glass, L., Hausdorff, J., Ivanov, P. C., Mark, R., ... & Stanley, H. E. (2000). PhysioBank, PhysioToolkit, and PhysioNet: Components of a new research resource for complex physiologic signals. Circulation [Online]. 101 (23), pp. e215–e220.
Abstract
The ECGRDVQ database contains multi-channel ECG recordings of 22 healthy subjects partaking in a randomized, double‐blind, 5‐period crossover clinical trial aimed at comparing the effects of four known QT prolonging drugs versus placebo on electrophysiological and other clinical parameters.
Experimental Method
In the morning of each period of the five 24-hour periods, each subject received a single dose of 500 μg dofetilide (Tikosyn, Pfizer, New York, NY), 400 mg quinidine sulfate (Watson Pharma, Corona, CA), 1500 mg ranolazine (Ranexa, Gilead, Foster City, CA), 120 mg verapamil hydrochloride (Heritage Pharmaceuticals, Edison, NJ) or placebo under fasting conditions. There was a 7-day washout period between each 24‐hour treatment period.
During each period, continuous ECGs were recorded at 500 Hz with an amplitude resolution of 2.5 μV. From the continuous recording, triplicate 10‐second ECGs were extracted at 16 predefined time-points: 1 point pre-dose (-0.5 h) and 15 points post-dose (0.5, 1, 1.5, 2, 2.5, 3, 3.5, 4, 5, 6, 7, 8, 12, 14, and 24 h), during which the subjects were resting in a supine position for 10 minutes.
At each of the 16 time-points, 3 optimal 10-second 12-lead ECGs were extracted with stable heart rates and maximum signal quality using Antares software (AMPS-LLC, New York City, NY). The resulting 5232 ECGs were up-sampled from 500 to 1000 Hz.
Files
The raw directory contains the 5232 original extracted 10-second standard 12 lead ECG segments organized in subdirectories named after the subject number or randomization number RANDID
in the second column of the SCR-002.Clinical.Data.csv file. The ECGs are stored in standard MIT format, with a signal .dat
file and corresponding header .hea
file for each segment
The medians directory contains derived representative median beats for 5223 of the 5232 raw ECG segments. Median beats were obtained as follows: the median PQRST waveform (median cardiac beat) for each lead was calculated by sample-by-sample synchronization of the QRS complex, and beats of a nonsinus origin were excluded based on a cross-correlation coefficient and RR interval history [1].
There are also semi-automatic annotations of each median beat based on the vector magnitude lead, containing P onset, QRS onset, QRS offset, T peak, secondary T peak (if present) and T offset. The annotations are stored in standard MIT annotation format, with annotator extension .atr
.
The SCR-002.Clinical.Data.csv file contains demographic information about the subjects, and important metadata about each ECG recording including their time-point, dosing period, associated drug, various beat intervals, and morphology measurements as described in Vicente et al. JAHA 2015. The spreadsheet column headings are described in the SCR-002.Clinical.Data.Description.txt file.
References
Additional Information
This data set, its source, and the methods used to generate it, are described in:
Johannesen L, Vicente J, Mason JW, Sanabria C, Waite-Labott K, Hong M, Guo P, Lin J, Sørensen JS, Galeotti L, Florian J, Ugander M, Stockbridge N, Strauss DG. Differentiating Drug-Induced Multichannel Block on the Electrocardiogram: Randomized Study of Dofetilide, Quinidine, Ranolazine, and Verapamil. Clin Pharmacol Ther. 2014 Jul 23. doi: 10.1038/clpt.2014.155.
The data set is also used in:
Vicente J, Johannesen L, Mason JW, Crumb WJ, Pueyo E, Stockbridge N, Strauss DG. Comprehensive T wave morphology assessment in a randomized clinical study of dofetilide, quinidine, ranolazine, and verapamil.doi: 10.1161/JAHA.114.001615.
ClinicalTrials.gov identifier: NCT01873950
Access
Access Policy:
Anyone can access the files, as long as they conform to the terms of the specified license.
License (for files):
Open Data Commons Attribution License v1.0
Discovery
DOI (version 1.0.0):
https://doi.org/10.13026/C2HP45
Topics:
medication
ecg
Corresponding Author
Files
Total uncompressed size: 1.4 GB.
Access the files
- Download the ZIP file (1.4 GB)
- Access the files using the Google Cloud Storage Browser here. Login with a Google account is required.
-
Access the data using the Google Cloud command line tools (please refer to the gsutil
documentation for guidance):
gsutil -m -u YOUR_PROJECT_ID cp -r gs://ecgrdvq-1.0.0.physionet.org DESTINATION
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Download the files using your terminal:
wget -r -N -c -np https://physionet.org/files/ecgrdvq/1.0.0/
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Download the files using AWS command line tools:
aws s3 sync --no-sign-request s3://physionet-open/ecgrdvq/1.0.0/ DESTINATION
Name | Size | Modified |
---|---|---|
medians | ||
raw | ||
ANNOTATORS (download) | 29 B | 2016-06-27 |
RECORDS (download) | 490.1 KB | 2016-08-18 |
SCR-002.Clinical.Data.Description.txt (download) | 1.9 KB | 2016-08-18 |
SCR-002.Clinical.Data.csv (download) | 1.2 MB | 2016-07-26 |
SHA256SUMS.txt (download) | 2.9 MB | 2019-02-20 |