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放射性标记 duramycin 靶向磷脂酰乙醇胺对缺血再灌注损伤中细胞凋亡的分子成像:有效摄取靶标,减少非靶器官的辐射负担。

Molecular Imaging of Apoptosis in Ischemia Reperfusion Injury With Radiolabeled Duramycin Targeting Phosphatidylethanolamine: Effective Target Uptake and Reduced Nontarget Organ Radiation Burden.

机构信息

Icahn School of Medicine at Mount Sinai, New York, New York.

Icahn School of Medicine at Mount Sinai, New York, New York.

出版信息

JACC Cardiovasc Imaging. 2018 Dec;11(12):1823-1833. doi: 10.1016/j.jcmg.2017.11.037. Epub 2018 Feb 14.

Abstract

OBJECTIVES

The purpose of this study was to evaluate the feasibility of imaging apoptosis in experimental ischemia-reperfusion model by technetium-99m (Tc)-labeled Duramycin, and compare it to an established tracer, Tc-labeled Annexin-V, which has a relative disadvantage of high radiation burden to nontarget organs.

BACKGROUND

During apoptosis, the cell membrane phospholipids-phosphatidylserine (PS) and phosphatidylethanolamine (PE) are exposed and can be targeted by Annexin-V and Duramycin, respectively, for in vivo imaging. Identification of a reversible cell death process should permit therapeutic intervention to help reduce myocyte loss and left ventricle dysfunction.

METHODS

In a 40-min left coronary artery ischemia-reperfusion model in 17 rabbits, 7 mCi of Tc-labeled Duramycin (n = 10), Tc-linear Duramycin (a negative tracer control; n = 3), or Tc-Annexin-V (a positive tracer-control; n = 4) were intravenously administered 30 min after reperfusion. Of the 10 Duramycin group animals, 4 animals were treated with an antiapoptotic agent, minocycline at the time of reperfusion. In vivo and ex vivo micro-single-photon emission computed tomography (μSPECT) and micro-computed tomography (μCT) imaging was performed 3 h after reperfusion, followed by quantitative assessment of tracer uptake and pathological characterization. Fluorescent Duramycin and Annexin-V were injected in 4 rats to visualize colocalization in infarct areas in a 40-min left coronary artery occlusion and 30-min reperfusion model.

RESULTS

Intense uptake of Duramycin and Annexin-V was observed in the apical (infarcted) areas. The percent injected dose per gram uptake of Duramycin in apical region (0.751 ± 0.262%) was significantly higher than remote area in same animals (0.045 ± 0.029%; p < 0.01). Duramycin uptake was insignificantly lower than Annexin-V uptake (1.23 ± 0.304%; p > 0.01) but demonstrated substantially lower radiation burden to kidneys (0.358 ± 0.210% vs. 1.58 ± 0.316%, respectively; p < 0.001). Fluorescence studies with Duramycin and Annexin V showed colocalization in infarct areas. Minocycline treatment substantially resolved Duramycin uptake (0.354% ± 0.0624%; p < 0.01).

CONCLUSIONS

Duramycin is similarly effective in imaging apoptotic cell death as Annexin-V with lower nontarget organ radiation. Clinical feasibility of apoptosis imaging with a PE-seeking tracer should be tested.

摘要

目的

本研究旨在通过锝-99m(Tc)标记的 Duramycin 评估在实验性缺血再灌注模型中成像细胞凋亡的可行性,并与已建立的示踪剂 Tc 标记的 Annexin-V 进行比较,后者对非靶器官具有相对较高的辐射负担的缺点。

背景

在细胞凋亡过程中,细胞膜磷脂酰丝氨酸(PS)和磷脂酰乙醇胺(PE)暴露,可以分别被 Annexin-V 和 Duramycin 靶向,用于体内成像。鉴定可逆的细胞死亡过程应该允许进行治疗干预,以帮助减少心肌细胞损失和左心室功能障碍。

方法

在 17 只兔子的 40 分钟左冠状动脉缺血再灌注模型中,再灌注后 30 分钟静脉注射 7 mCi 的 Tc 标记 Duramycin(n=10)、Tc 线性 Duramycin(阴性示踪剂对照;n=3)或 Tc-Annexin-V(阳性示踪剂对照;n=4)。在 Duramycin 组的 10 只动物中,有 4 只动物在再灌注时接受了一种抗凋亡药物米诺环素的治疗。再灌注后 3 小时进行体内和体外微单光子发射计算机断层扫描(μSPECT)和微计算机断层扫描(μCT)成像,并对示踪剂摄取进行定量评估和病理特征分析。在 40 分钟左冠状动脉闭塞和 30 分钟再灌注模型中,将荧光标记的 Duramycin 和 Annexin-V 注射到 4 只大鼠中,以可视化梗死区域的共定位。

结果

在顶部(梗死)区域观察到 Duramycin 和 Annexin-V 的强烈摄取。顶端区域 Duramycin 的注射剂量百分比摄取(0.751±0.262%)明显高于同一动物的远程区域(0.045±0.029%;p<0.01)。Duramycin 的摄取量略低于 Annexin-V 的摄取量(1.23±0.304%;p>0.01),但对肾脏的辐射负担明显较低(分别为 0.358±0.210%和 1.58±0.316%;p<0.001)。Duramycin 和 Annexin V 的荧光研究显示在梗死区域有共定位。米诺环素治疗可显著降低 Duramycin 的摄取量(0.354%±0.0624%;p<0.01)。

结论

Duramycin 在成像细胞凋亡方面与 Annexin-V 同样有效,对非靶器官的辐射较低。应该测试使用 PE 靶向示踪剂进行细胞凋亡成像的临床可行性。

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