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Heart 2002;87:205-209 doi:10.1136/heart.87.3.205
  • Cardiovascular medicine

Virtual coronary angioscopy using multislice computed tomography

  1. S Schroeder1,
  2. A F Kopp2,
  3. B Ohnesorge3,
  4. H Loke-Gie3,
  5. A Kuettner1,
  6. A Baumbach4,
  7. C Herdeg1,
  8. C D Claussen2,
  9. K R Karsch4
  1. 1Department of Internal Medicine, Division of Cardiology Eberhard-Karls-University, Tuebingen, Germany
  2. 2Department of Radiology, Division of Diagnostic Radiology, Eberhard-Karls-University
  3. 3Siemens AG, Medical Engineering, Computed Tomography, Forchheim, Germany
  4. 4Department of Cardiology, Bristol Heart Institute, University of Bristol, United Kingdom
  1. Correspondence to:
    Dr Stephen Schroeder, Medical Clinic, Division of Cardiology, University of Tuebingen, Otfried-Mueller-Strasse 10, D-72076 Tuebingen, Germany;
    stephen.schroeder{at}med.uni-tuebingen.de
  • Accepted 26 September 2001

Abstract

Background: With faster image acquisition times and thinner slice widths, multislice detector computed tomography (MSCT) allows visualisation of human coronary arteries with diagnostic image quality. In addition to conventional axial slices, virtual coronary angioscopies (VCA) can be reconstructed using MSCT datasets.

Objective: To evaluate the feasibility of reconstructing VCA and to determine the clinical value of this new application in detecting atherosclerotic coronary artery lesions.

Methods: Datasets obtained by contrast enhanced non-invasive coronary angiography using MSCT (Somatom VZ) were analysed from 14 consecutive patients. VCA were simulated in 14 coronary arteries (left anterior descending, n = 7; right coronary, n = 7). Lesion detection was undertaken on conventional contrast enhanced axial slices, as well as by VCA. Intracoronary ultrasound (ICUS) was used as the gold standard for in vivo plaque detection.

Results: 38 lesions were detected both on ICUS and on axial slices: 14 severe target lesions of > 75% area stenosis (11 calcified, three non-calcified), and 24 intermediate lesions of ≤ 75% area stenosis (seven calcified, 17 non-calcified). Using VCA, all severe lesions (n = 14) and all calcified intermediate plaques (n = 7) could clearly be identified. However, non-calcified intermediate lesions (n = 17) could not be accurately distinguished from the vessel wall; they were recognised as vessel wall alterations without significant luminal narrowing.

Conclusions: Current MSCT technology allows reconstruction of VCA with good image quality. Despite a more anatomical view of heart and coronary vessels on three dimensional reconstruction, conventional axial slices were found to be superior for detecting coronary lesions. Thus further technical innovations are required before VCA can become a useful technique in clinical cardiology.

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