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心脏发射计算机断层扫描:由于壁运动异常导致局部示踪剂浓度低估。

Cardiac emission computed tomography: underestimation of regional tracer concentrations due to wall motion abnormalities.

作者信息

Parodi O, Schelbert H R, Schwaiger M, Hansen H, Selin C, Hoffman E J

出版信息

J Comput Assist Tomogr. 1984 Dec;8(6):1083-92.

PMID:6334106
Abstract

Possible effects of regional wall motion abnormalities on apparent regional myocardial tracer concentrations on emission tomographic images were evaluated in six open chest dogs. Each dog was studied twice: In Run 1, 13N ammonia and microspheres were injected during a 6 min coronary occlusion, and serial images acquired by positron emission tomography during occlusion and reperfusion. In Run 2, 1 h later, 13N ammonia and microspheres were reinjected at control, and serial images recorded at control, during a repeat 6 min coronary occlusion, and after reperfusion. Segmental function was monitored with ultrasonic crystals, and 13N tissue concentrations determined in vivo from the tomographic images and postmortem by well counting. In Run 1, fractional shortening in ischemic segments fell by 89 +/- 16% SD from control. The ischemic versus control segment ratio for 13N activity concentrations averaged 0.29 +/- 0.08 and for microspheres 0.20 +/- 0.15. In Run 2 the ischemic versus control segment ratio was at control 0.77 +/- 0.12 for 13N tissue activity and 0.85 +/- 0.07 for microspheres. Fractional shortening fell during occlusion by 131 +/- 29% from control, returned to control early, and fell again by 11 +/- 16% late during reperfusion. These changes were paralleled by changes in apparent regional 13N tissue concentrations of the prelabeled myocardium. Compared with control, they were 37 +/- 9% lower during occlusion and rose to 94 +/- 20% early and to 89 +/- 16% at control late during reperfusion. In vitro determined tissue concentration ratios of ischemic to control myocardium were similar for 13N and microsphere activity (0.83 and 0.85), which ruled out loss of 13N ammonia from tissue during occlusion or reperfusion. Our results indicate that regional wall motion abnormalities cause artifactual segmental defects in tracer concentrations on emission tomographic images of the heart, which must be considered for qualitative and quantitative analysis of regional tracer tissue concentrations.

摘要

在六只开胸犬中评估了局部室壁运动异常对发射断层图像上局部心肌示踪剂浓度的可能影响。每只犬均进行了两次研究:在实验1中,在6分钟冠状动脉闭塞期间注射13N氨和微球,并在闭塞和再灌注期间通过正电子发射断层扫描获取系列图像。在1小时后的实验2中,以对照状态再次注射13N氨和微球,并在对照状态、重复的6分钟冠状动脉闭塞期间以及再灌注后记录系列图像。用超声晶体监测节段功能,并通过断层图像在体内以及死后通过井型计数法测定13N组织浓度。在实验1中,缺血节段的缩短分数较对照下降了89±16%(标准差)。13N活性浓度的缺血节段与对照节段之比平均为0.29±0.08,微球的该比值为0.20±0.15。在实验2中,13N组织活性的缺血节段与对照节段之比在对照状态下为0.77±0.12,微球的该比值为0.85±0.07。闭塞期间缩短分数较对照下降了131±29%,早期恢复到对照水平,再灌注后期再次下降11±16%。这些变化与预先标记心肌的局部13N组织浓度的变化平行。与对照相比,闭塞期间降低了37±9%,再灌注早期升至94±20%,再灌注后期降至对照水平的89±16%。体外测定的缺血心肌与对照心肌的组织浓度比对于13N和微球活性相似(分别为0.83和0.85),这排除了在闭塞或再灌注期间13N氨从组织中丢失的情况。我们的结果表明,局部室壁运动异常会在心脏发射断层图像上的示踪剂浓度中导致人为的节段性缺损,在对局部示踪剂组织浓度进行定性和定量分析时必须考虑到这一点。

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