锝99m N - NOET在正常、缺血再灌注及细胞膜破坏的心肌中的清除情况。
Clearance of technetium 99m N-NOET in normal, ischemic-reperfused, and membrane-disrupted myocardium.
作者信息
Johnson G, Allton I L, Nguyen K N, Lauinger J M, Beju D, Pasqualini R, Duatti A, Okada R D
机构信息
William K. Warren Medical Research Institute, University of Oklahoma Health Sciences Center, Tulsa 74136, USA.
出版信息
J Nucl Cardiol. 1996 Jan-Feb;3(1):42-54. doi: 10.1016/s1071-3581(96)90023-9.
BACKGROUND
Technetium 99m-labeled bis(N-ethoxy, N-ethyl dithiocarbamato) nitrido technetium(v) (99mTcN-NOET) is a new neutral cardiac perfusion imaging agent that has been shown to have very high uptake and retention in vitro. The purpose of this study was to determine the clearance kinetics of 99mTcN-NOET in control, ischemic-reperfused, and membrane-disrupted myocardium.
METHODS AND RESULTS
After a 100 microCi (3.7 x 10(6) Bq) bolus of 99mTcN-NOET was injected, myocardial clearance was monitored for 1 hour by the use of a sodium iodide detector in 30 isolated, Krebs-Henseleit (KH) perfused rat hearts. Seven hearts were used as controls (group 1). In seven ischemic-reperfused hearts, tracer administration and uptake was followed by 30 minutes of no flow and 1 hour of reflow (group 2). In six additional ischemic-reperfused hearts, tracer administration was followed by deprivation of flow for 1 hour followed by 1 hour of reflow (group 3). Six hearts were perfused with a 0.5% Triton X-100 KH perfusate for 1 hour (group 4). Four hearts were perfused with KH for 10 minutes, followed by cyanide for 10 minutes (group 5). This cycle was repeated three times. Activities remaining in each heart at the end of each experiment were quantitated, and activity at peak uptake was calculated. The 99mTcN-NOET myocardial clearance was near linear in the control (0.6 +/- 0.4) and both ischemic-reperfused groups with virtually no fractional clearance (1.2% +/- 0.6% and 2.1% +/- 0.6%, respectively; p = NS). In the Triton X-100 membrane-disrupted hearts, clearance was substantial (94.2% +/- 4.0%; p < 0.0001 compared with the control and ischemic-reperfused groups). Cyanide treatment produced rapid clearance, which was arrested by a return to the standard KH perfusate. Peak uptake as a percentage of injected dose was 74.9% +/- 1.4% for all groups combined.
CONCLUSION
Thus 99mTcN-NOET has extremely high myocardial retention after 1 hour in normal myocardium and is not significantly affected by ongoing myocardial ischemia or reperfusion injury in this model. Clearance is increased markedly in extreme conditions of membrane disruption. These data are consistent with the concept that 99mTc-NOET is localized predominantly in or on cell membranes. 99mTcN-NOET is a promising, new myocardial perfusion imaging agent that exhibits a stable myocardial distribution in the setting of acute developing injury.
背景
锝99m标记的双(N - 乙氧基,N - 乙基二硫代氨基甲酸盐)氮鎝(Ⅴ)(99mTcN - NOET)是一种新型中性心脏灌注显像剂,已证实在体外具有非常高的摄取和滞留率。本研究的目的是确定99mTcN - NOET在对照、缺血再灌注和膜破坏心肌中的清除动力学。
方法与结果
在注射100微居里(3.7×10⁶贝克勒尔)的99mTcN - NOET推注后,使用碘化钠探测器在30个离体的、用克雷布斯 - 亨塞尔特(KH)灌注的大鼠心脏中监测心肌清除1小时。7个心脏用作对照(第1组)。在7个缺血再灌注心脏中,注入示踪剂并摄取后,进行30分钟无血流和1小时再灌注(第2组)。在另外6个缺血再灌注心脏中,注入示踪剂后进行1小时无血流,然后再灌注1小时(第3组)。6个心脏用0.5% Triton X - 100 KH灌注液灌注1小时(第4组)。4个心脏用KH灌注10分钟,然后用氰化物灌注10分钟(第5组)。这个循环重复3次。在每个实验结束时对每个心脏中剩余的活性进行定量,并计算摄取峰值时的活性。99mTcN - NOET心肌清除在对照组(0.6±0.4)以及两个缺血再灌注组中接近线性,几乎没有分数清除(分别为1.2%±0.6%和2.1%±0.6%;p =无显著性差异)。在Triton X - 100膜破坏的心脏中清除显著(94.2%±4.0%;与对照组和缺血再灌注组相比,p < 0.0001)。氰化物处理导致快速清除,恢复到标准KH灌注液后清除停止。所有组的摄取峰值占注射剂量的百分比为74.9%±1.4%。
结论
因此,99mTcN - NOET在正常心肌中1小时后具有极高的心肌滞留率,并且在该模型中不受持续的心肌缺血或再灌注损伤的显著影响。在膜破坏的极端情况下清除明显增加。这些数据与99mTc - NOET主要定位于细胞膜内或细胞膜上的概念一致。99mTcN - NOET是一种有前景的新型心肌灌注显像剂,在急性发展性损伤情况下表现出稳定的心肌分布。
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