Abstract
The complexity of a heart rate variability (HRV) signal is considered an important nonlinear feature to detect cardiac abnormalities. This work aims at explaining the physiological meaning of a recently developed complexity measurement method, namely, distribution entropy (DistEn), in the context of HRV signal analysis. We thereby propose modified distribution entropy (mDistEn) to remove the physiological discrepancy involved in the computation of DistEn. The proposed method generates a distance matrix that is devoid of over-exerted multi-lag signal changes. Restricted element selection in the distance matrix makes “mDistEn” a computationally inexpensive and physiologically more relevant complexity measure in comparison to DistEn.
Funder
National Natural Science Foundation of China
Australian Research Council
Subject
General Physics and Astronomy
Cited by
6 articles.
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