4.5 Article

Whole heart detailed and quantitative anatomy, myofibre structure and vasculature from X-ray phase-contrast synchrotron radiation-based micro computed tomography

Journal

EUROPEAN HEART JOURNAL-CARDIOVASCULAR IMAGING
Volume 18, Issue 7, Pages 732-741

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/ehjci/jew314

Keywords

myocardial remodelling; myofibre structure; coronary vasculature; synchrotron phase-contrast CT

Funding

  1. Ministerio de Economia y Competitividad [SAF2012-37196, TIN2014-52923-R]
  2. Instituto de Salud Carlos III integrados en el Plan Nacional de I+D+I y cofinanciados por el ISCIII-Subdireccion General de Evaluacion y el Fondo Europeo de Desarrollo Regional (FEDER) 'Otra manera de hacer Europa' [PI11/00051, PI11/01709, PI12/00801, PI14/00226]
  3. EU for research, technological development and demonstration under VP2HF [611823]
  4. Cerebra Foundation for the Brain Injured Child (Carmarthen, UK)
  5. Obra Social 'la Caixa' (Barcelona, Spain)
  6. Fundacio Mutua Madrilena and Fundacio Agrupacio Mutua (Spain)

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Background While individual cardiac myocytes only have a limited ability to shorten, the heart efficiently pumps a large volume-fraction thanks to a cell organization in a complex 3D fibre structure. Subclinical subtle cardiac structural remodelling is often present before symptoms arise. Understanding and early detection of these subtle changes is crucial for diagnosis and prevention. Additionally, personalized computational modelling requires knowledge on the multi-scale structure of the whole heart and vessels. Methods and results We developed a rapid acquisition together with visualization and quantification methods of the integrated microstructure of whole in-vitro rodents hearts using synchrotron based X-ray phase-contrast tomography. These images are formed not only by X-ray absorption by the tissue but also by wave propagation phenomena, enhancing structural information, thus allowing to raise tissue contrast to an unprecedented level. We used a (ex-vivo) normal rat heart and fetal rabbit hearts suffering intrauterine growth restriction as a model of subclinical cardiac remodelling to illustrate the strengths and potential of the technique. For comparison, histology and diffusion tensor magnetic resonance imaging was performed. Conclusions We have developed a novel, high resolution, image acquisition, and quantification approach to study a whole in-vitro heart at myofibre resolution, providing integrated 3D structural information at microscopic level without any need of tissue slicing and processing. This superior imaging approach opens up new possibilities for a systems approach towards analysing cardiac structure and function, providing rapid acquisition of quantitative microstructure of the heart in a near native state.

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