Multiscale entropy of laser Doppler flowmetry signals in healthy human subjects

被引:22
|
作者
Humeau, Anne [1 ,4 ]
Buard, Benjamin [1 ,2 ]
Mahe, Guillaume [3 ]
Rousseau, David [1 ]
Chapeau-Blondeau, Francois [1 ]
Abraham, Pierre
机构
[1] Univ Angers, LISA, F-49000 Angers, France
[2] Grp Esaip, F-49180 St Barthelemy Anjou, France
[3] CHU Angers, Lab Physiol & Explorat Vasc, UMR CNRS 6214, INSERM 771, F-49033 Angers 01, France
[4] Univ Angers, LISA, Inst Univ Technol, Dept GEII, F-49016 Angers, France
关键词
laser Doppler flowmetry; microcirculation; multiscale entropy; PERIPHERAL CARDIOVASCULAR-SYSTEM; PHASE-SPACE APPROACH; TISSUE BLOOD-FLOW; APPROXIMATE ENTROPY; SAMPLE ENTROPY; REACTIVE HYPEREMIA; TIME-SERIES; COMPLEXITY; SKIN; MULTIFRACTALITY;
D O I
10.1118/1.3512796
中图分类号
R8 [特种医学]; R445 [影像诊断学];
学科分类号
1002 ; 100207 ; 1009 ;
摘要
Purpose: The cardiovascular system (CVS) regulation can be studied from a central viewpoint, through heart rate variability (HRV) data, and from a peripheral viewpoint, through laser Doppler flowmetry (LDF) signals. Both the central and peripheral CVSs are regulated by several interacting mechanisms, each having its own temporal scale. The central CVS has been the subject of many multiscale studies. By contrast, these studies at the level of the peripheral CVS are very recent. Among the multiscale studies performed on the central CVS data, multiscale entropy has been proven to give interesting physiological information for diagnostic purposes. However, no multiscale entropy analysis has been performed on LDF signals. The authors' goal is therefore to propose a first multiscale entropy study of LDF data recorded in healthy subjects. Methods: The LDF signals recorded in the forearm of seven healthy subjects are processed. Their period sampling is T=50 ms, and coarse-graining scales from T to 23T are studied. Also, for validation, the algorithm is first tested on synthetic signals of known theoretical multiscale entropy. Results: The results reveal nonmonotonic evolution of the multiscale entropy of LDF signals, with a maximum at small scales around 7T and a minimum at longer scales around 18T, singling out in this way two distinctive scales where the LDF signals undergo specific changes from high to low complexity. This also marks a strong contrast with the HRV signals that usually display a monotonic increase in the evolution of the multiscale entropy. Conclusions: Multiscale entropy of LDF signals in healthy subjects shows variation with scales. Moreover, as the variation pattern observed appears similar for all the tested signals, multiscale entropy could potentially be a useful stationary signature for LDF signals, which otherwise are probe-position and subject dependent. Further work could now be conducted to evaluate possible diagnostic purposes of the multiscale entropy of LDF signals. (C) 2010 American Association of Physicists in Medicine. [DOI: 10.1118/1.3512796]
引用
收藏
页码:6142 / 6146
页数:5
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