| Literature DB >> 32161769 |
Nathan Angel1,2, Eugene G Kholmovski3,4, Elyar Ghafoori1,2,5, Derek J Dosdall2,5,6, Rob S MacLeod1,2,5, Ravi Ranjan1,2,5.
Abstract
Regions within the atria with sustained rapid reentrant or focal activity have been defined as a mechanism of persistent atrial fibrillation (AF). However, the mechanism behind the anchoring of these sites and their stability over time is unknown. We tested the hypothesis that fibrosis anchors sites of high frequency activation during AF and that these sites can be non-invasively determined using cardiac T1 Mapping with MRI. A canine rapid atrial paced model of persistent AF was used (n=12, including 6 controls) for the study. Whole heart T1 Mapping was performed prior to an electrical mapping study. Spatial maps of high dominant frequency (DF) probability were constructed to determine stability of the highest DF sites. These sites were then correlated with fibrotic regions determined by T1 Mapping. The chronic AF animals had at least one site of stable, high DF for at least 22.5 (75%) of 30 minutes of AF. Regions of stable high DF bordered regions of fibrosis as determined by T1 Mapping MRI 82% of the time (p<0.05). Heterogeneous atrial remodeling, specifically fibrosis, arising from chronic AF may provide a substrate that anchors sites of high DF. Cardiac T1 Mapping with MRI may determine such sites non-invasively.Entities:
Year: 2020 PMID: 32161769 PMCID: PMC7065674 DOI: 10.22489/cinc.2019.403
Source DB: PubMed Journal: Comput Cardiol (2010) ISSN: 2325-887X