期刊
JOURNAL OF NUCLEAR MEDICINE
卷 52, 期 6, 页码 965-969出版社
SOC NUCLEAR MEDICINE INC
DOI: 10.2967/jnumed.110.085993
关键词
autoradiography; animal imaging; cardiology (basic/technical); molecular imaging; PET
资金
- 2008 Nuclear Cardiology Foundation
- American Heart Association
- National Institutes of Health [1RO1HL092985]
F-18-fluorobenzyl triphenyl phosphonium (FBnTP) has recently been introduced as a myocardial perfusion PET agent. We used a rat model of transient coronary occlusion to determine the stability of the perfusion defect size over time and the magnitude of redistribution. Methods: Wistar rats (n = 15) underwent thoracotomy and 2-min occlusion of the left coronary artery (LCA), followed by reperfusion. During occlusion, F-18-FBnTP (92.5 MBq) and Tl-201-thallium chloride (0.74 MBq) were injected intravenously. One minute before the animals were sacrificed at 5, 45, and 120 min after reperfusion, the LCA was occluded again and 2% Evans blue was injected intravenously to determine the ischemic territory. The hearts were excised, frozen, and sliced for serial dual-tracer autoradiography and histology. Dynamic in vivo F-18-FBnTP PET was performed on a subgroup of animals (n = 4). Results: F-18-FBnTP showed stable ischemic defects at all time points after tracer injection and reperfusion. The defects matched the blue dye defect (y = 0.97x +1.5, R-2 = 0.94, y = blue-dye defect, x = F-18-FBnTP defect). Count density analysis showed no defect fill-in at 45 min but slightly increased activity at 120 min (LCA/remote uptake ratio = 0.19 +/- 0.02, 0.19 +/- 0.05, and 0.34 +/- 0.06 at 5, 45, and 120 min, respectively, P < 0.05). For comparison, Tl-201 showed complete redistribution at 120 min (LCA/remote = 0.42 +/- 0.04, 0.72 +/- 0.03, and 0.97 +/- 0.05 at 5, 45, and 120 min, respectively, P < 0.001). Persistence of the F-18-FBnTP defect over time was confirmed by in vivo dynamic small-animal PET. Conclusion: In a transient coronary occlusion model, perfusion defect size using the new PET agent F-18-FBnTP remained stable for at least 45 min and matched the histologically defined ischemic area. This lack of significant redistribution suggests a sufficient time window for future clinical protocols with tracer injection remote from the scanner, such as in a stress testing laboratory or chest pain unit.
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