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缺氧显像剂[I]IAZA在健康成年人运动负荷心脏应激后的药代动力学及闪烁显像†

Pharmacokinetics and Scintigraphic Imaging of the Hypoxia-Imaging Agent [I]IAZA in Healthy Adults Following Exercise-Based Cardiac Stress †.

作者信息

Stypinski Daria, McQuarrie Stephen A, McEwan Alexander J B, Wiebe Leonard I

机构信息

Pfizer Inc., Clinical Pharmacokinetics, Pfizer Inc., New York, NY 10017, USA.

PET Centre, Department of Oncology, University of Alberta, 11560 University Ave, Edmonton, AB T6B 1Z2, Canada.

出版信息

Pharmaceutics. 2018 Feb 22;10(1):25. doi: 10.3390/pharmaceutics10010025.

Abstract

The objective of this work is to evaluate the potential effect of cardiac stress exercise on the accumulation of [I]IAZA, a radiopharmaceutical used to image focal tissue hypoxia, in otherwise normal myocardium in healthy volunteers, and to determine the impact of exercise on [I]IAZA pharmacokinetics. The underlying goal is to establish a rational basis and a baseline for studies of focal myocardial hypoxia in cardiac patients using [I]IAZA. Three healthy male volunteers ran the 'Bruce' treadmill protocol, a clinically-accepted protocol designed to expose myocardial ischemia in patients. The 'Bruce' criterion heart rate is 85% of [220-age]. Approximately one minute before reaching this level, [I]IAZA (5.0 mCi/0.85 mg) was administered as a slow (1-3 min) single intravenous (i.v.) injection via an indwelling venous catheter. The volunteer continued running for an additional 1 min before being transferred to a gamma camera. Serum samples were collected from the arm contralateral to the administration site at pre-determined intervals from 1 min to 45 h post injection and were analyzed by radio HPLC. Pharmacokinetic (PK) parameters were derived for [I]IAZA and total radioactivity (total[I]) using compartmental and noncompartmental analyses. Whole-body planar scintigraphic images were acquired from 0.75 to 24 h after dosing. PK data and scintigraphic images were compared to previously published [I]IAZA data from healthy volunteers rest. Following exercise stress, both [I]IAZA and total[I] exhibited bi-exponential decline profiles, with rapid distribution phases [half-lives (t) of 1.2 and 1.4 min, respectively], followed by slower elimination phases [t of 195 and 290 min, respectively]. Total body clearance (CL) and the steady state volume of distribution (V) were 0.647 L/kg and 185 mL/min, respectively, for [I]IAZA and 0.785 L/kg and 135 mL/min, respectively, for total[I]. The t, CL and V values were comparable to those reported previously for rested volunteers. The t was approximately 4-fold shorter for [I]IAZA and approximately 3-fold shorter for total[I] under exercise relative to rested subjects. The heart region was visualized in early whole body scintigraphic images, but later images showed no accumulated radioactivity in this region, and no differences from images reported for rested volunteers were apparent. Minimal uptake of radiotracer in myocardium and skeletal muscle was consistent with uptake in non-stressed myocardium. Whole-body scintigrams for [I]IAZA in exercise-stressed healthy volunteers were indistinguishable from images of non-exercised volunteers. There was no evidence of hypoxia-dependent binding in exercised but otherwise healthy myocardium, supporting the conclusion that exercise stress at Bruce protocol intensity does not induce measurable myocardial hypoxia. Effects of exercise on PK parameters were minimal; specifically, the t was shortened, reflecting increased cardiac output associated with exercise. It is concluded that because [I]IAZA was not metabolically bound in exercise-stressed myocardium, a stress test will not create elevated myocardial background that would mask regions of myocardial perfusion deficiency. [I]IAZA would therefore be suitable for the detection of viable, hypoxic myocardium in patients undergoing stress-test-based diagnosis.

摘要

本研究的目的是评估心脏应激运动对健康志愿者正常心肌中用于成像局部组织缺氧的放射性药物[I]IAZA蓄积的潜在影响,并确定运动对[I]IAZA药代动力学的影响。其根本目标是为使用[I]IAZA研究心脏病患者局部心肌缺氧建立合理依据和基线。三名健康男性志愿者按照“布鲁斯”跑步机方案进行运动,该方案是临床上用于使患者暴露心肌缺血的公认方案。“布鲁斯”标准心率为[220 - 年龄]的85%。在达到该水平前约一分钟,通过留置静脉导管以缓慢(1 - 3分钟)单次静脉注射的方式给予[I]IAZA(5.0毫居里/0.85毫克)。志愿者继续跑步1分钟后被转移至伽马相机。在注射后1分钟至45小时的预定时间间隔,从给药部位对侧手臂采集血清样本,并通过放射性高效液相色谱法进行分析。使用房室分析和非房室分析得出[I]IAZA和总放射性(总[I])的药代动力学(PK)参数。给药后0.75至24小时采集全身平面闪烁扫描图像。将PK数据和闪烁扫描图像与先前发表的健康志愿者静息状态下的[I]IAZA数据进行比较。运动应激后,[I]IAZA和总[I]均呈现双指数下降曲线,快速分布相[半衰期(t)分别为1.2分钟和1.4分钟],随后是较慢的消除相[t分别为195分钟和290分钟]。[I]IAZA的全身清除率(CL)和稳态分布容积(V)分别为0.647升/千克和185毫升/分钟,总[I]的分别为0.785升/千克和135毫升/分钟。这些t、CL和V值与先前报道的静息志愿者的值相当。与静息受试者相比,运动状态下[I]IAZA的t约短4倍,总[I]的t约短3倍。在早期全身闪烁扫描图像中可看到心脏区域,但后期图像显示该区域无放射性蓄积,且与静息志愿者报告的图像无明显差异。心肌和骨骼肌中放射性示踪剂的摄取极少,这与非应激心肌中的摄取情况一致。运动应激的健康志愿者的[I]IAZA全身闪烁扫描图与未运动志愿者的图像无差异。在运动但其他方面健康的心肌中没有缺氧依赖性结合的证据,支持以下结论:按照布鲁斯方案强度进行的运动应激不会诱导可测量的心肌缺氧。运动对PK参数的影响极小;具体而言,t缩短,反映了与运动相关的心输出量增加。得出结论,由于[I]IAZA在运动应激的心肌中未发生代谢结合,应激试验不会产生会掩盖心肌灌注不足区域的心肌背景升高。因此,[I]IAZA适用于在基于应激试验的诊断中检测存活的缺氧心肌。

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