Quantification of viable myocardium in multivessel coronary disease: Effects of the redistribution time after reinjection of thallium-201 and comparison with postrevascularization defect size

Uwe Helber; Wolfgang Müller-Schauenburg; Hans Martin Hoffmeister

doi:10.1007/BF01616841

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Int J Angiol 1999; 8(1): 36-39
DOI: 10.1007/BF01616841

Original Articles

Quantification of viable myocardium in multivessel coronary disease: Effects of the redistribution time after reinjection of thallium-201 and comparison with postrevascularization defect size

Uwe Helber¹ , Wolfgang Müller-Schauenburg² , Hans Martin Hoffmeister¹

¹Medizinische Klinik Abt. III, Eberhard-Karls-Universität, Tübingen, Germany
²Abt. für Nuklearmedizin, Eberhard-Karls-Universität, Röntgenweg, D-72076, Tübingen, Germany

Presented in part at the 39th Annual World Congress, International College of Angiology, Istanbul, Turkey, June 1997

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Publication Date:
24 April 2011 (online)

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Abstract

Reinjection of²⁰¹Tl is used for improved detection of viable myocardium. Prospectively the effect of the redistribution time after injection for the quantification of the definitive perfusion defect size in multivessel coronary heart disease and severely impaired left ventricular function was examined. Thirty patients were included preoperatively before CABG. The study was performed with 80–90 MBq²⁰¹Tl-Cl and reinjection (40–50 MBq). Imaging was performed after an exercise test and 3 hours afterwards. Thereafter, the reinjection dose was given and repeated studies were performed 10 minutes, 2 hours, and 20 hours later. Defect sizes were compared with the 3-hour rest-study without reinjection. Imaging studies were repeated postoperatively. The defect size was expressed as % of left ventricular total myocardium. Perfusion defect sizes were as follows: post-stress study (27%), 3 hour rest-study (17%), post-reinjection-10 min (12%), 2 hours (9%), and 20 hours (7%). Compared with the 3 hour rest-study, the perfusion defect was reduced only in 7/30 patients in the study immediately after reinjection. In the delayed studies, defect sizes were markedly smaller (p <0.05) both in studies 2 hours and 20 hours after reinjection. In 15/30 patients there was a marked reduction of 50% of defect sizes in the study 2 hours post-reinjection vs the 3 hour rest-study. The residual defects at 2 hours after reinjection were identical to the postoperative defect sizes (10%). Further prolongation of the redistribution time to 20 horus caused an additional small reduction in defect size only in two patients compared with the 2-hour post-reinjection images (n.s.). Using a marker as²⁰¹Tl with redistribution characteristics, the redistribution time after reinjection is of utmost importance to correctly identify the definitive size of the perfusion defect vs viable myocardium in patients with multivessel disease. A delay of 2 hours for redistribution after the reinjection most correctly corresponds to the postop defect size; a longer redistribution time did not provide additional advantages.

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