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Applicability of the single equivalent point dipole model to represent a spatially distributed bio-electrical sourceAlthough the single equivalent point dipole model has been used to represent well-localised bio-electrical sources, in realistic situations the source is distributed. Consequently, position estimates of point dipoles determined by inverse algorithms suffer from systematic error due to the non-exact applicability of the inverse model. In realistic situations, this systematic error cannot be avoided, a limitation that is independent of the complexity of the torso model used. This study quantitatively investigates the intrinsic limitations in the assignment of a location to the equivalent dipole due to distributed electrical source. To simulate arrhythmic activity in the heart, a model of a wave of depolarisation spreading from a focal source over the surface of a spherical shell is used. The activity is represented by a sequence of concentric belt sources (obtained by slicing the shell with a sequence of parallel plane pairs), with constant dipole moment per unit length (circumferentially) directed parallel to the propagation direction. The distributed source is represented by N dipoles at equal arc lengths along the belt. The sum of the dipole potentials is calculated at predefined electrode locations. The inverse problem involves finding a single equivalent point dipole that best reproduces the electrode potentials due to the distributed source. The inverse problem is implemented by minimising the chi2 per degree of freedom. It is found that the trajectory traced by the equivalent dipole is sensitive to the location of the spherical shell relative to the fixed electrodes. It is shown that this trajectory does not coincide with the sequence of geometrical centres of the consecutive belt sources. For distributed sources within a bounded spherical medium, displaced from the sphere's centre by 40% of the sphere's radius, it is found that the error in the equivalent dipole location varies from 3 to 20% for sources with size between 5 and 50% of the sphere's radius. Finally, a method is devised to obtain the size of the distributed source during the cardiac cycle.
Document ID
20040088637
Acquisition Source
Legacy CDMS
Document Type
Reprint (Version printed in journal)
Authors
Armoundas, A. A.
(Harvard University-Massachusetts Institute of Technology, Division of Health Sciences & Technology Cambridge, United States)
Feldman, A. B.
Sherman, D. A.
Cohen, R. J.
Date Acquired
August 21, 2013
Publication Date
September 1, 2001
Publication Information
Publication: Medical & biological engineering & computing
Volume: 39
Issue: 5
ISSN: 0140-0118
Subject Category
Life Sciences (General)
Funding Number(s)
CONTRACT_GRANT: HL09570
Distribution Limits
Public
Copyright
Other
Keywords
NASA Discipline Cardiopulmonary
Non-NASA Center

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