There has been an increasing interest in studying cardiac fibers in order to improve the current knowledge regarding the mechanical and physiological properties of the heart during heart failure (HF), particularly early HF. Having a thorough understanding of the changes in cardiac fiber orientation may provide new insight into the mechanisms behind the progression of left ventricular (LV) remodeling and HF. We conducted a systematic review on various technologies for imaging cardiac fibers and its link to HF. This review covers literature reports from 1900 to 2017. PubMed and Google Scholar databases were searched using the keywords “cardiac fiber” and “heart failure” or “myofiber” and “heart failure.” This review highlights imaging methodologies, including magnetic resonance diffusion tensor imaging (MR-DTI), ultrasound, and other imaging technologies as well as their potential applications in basic and translational research on the development and progression of HF. MR-DTI and ultrasound have been most useful and significant in evaluating cardiac fibers and HF. New imaging technologies that have the ability to measure cardiac fiber orientations and identify structural and functional information of the heart will advance basic research and clinical diagnoses of HF.
Purpose To develop a robust method to assess regional mechanical dyssynchrony from cine short-axis MR images. Cardiac resynchronization therapy (CRT) is an effective treatment for patients with heart failure and evidence of left-ventricular (LV) dyssynchrony. Patient response to CRT is greatest when the LV pacing lead is placed in the most dyssynchronous segment. Existing techniques for assessing regional dyssynchrony require difficult acquisition and/or postprocessing. Our goal was to develop a widely applicable and robust method to assess regional mechanical dyssynchrony. Materials and Methods Using the endocardial boundary, radial displacement curves (RDCs) were generated throughout the LV. Cross-correlation was used to determine the delay time between each RDC and a patient-specific reference. Delay times were projected onto the American Heart Association 17-segment model creating a regional dyssynchrony map. Our method was tested in 10 normal individuals and 10 patients enrolled for CRT (QRS > 120 ms, NYHA III-IV, EF < 35%). Results Delay times over the LV were 23.9 ± 33.8 ms and 93.1 ± 99.9 ms (P < 0.001) in normal subjects and patients, respectively. Interobserver reproducibility for segment averages was 6.8 ± 39.3 ms and there was 70% agreement in identifying the latest contracting segment. Conclusion We have developed a method that can reliably calculate regional delay times from cine steady-state free-precession (SSFP) images. Maps of regional dyssynchrony could be used to identify the latest-contracting segment to assist in CRT lead implantation.