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Assessing cardiac injury in mice with dual energy-microCT, 4D-microCT, and microSPECT imaging after partial heart irradiation.

机译:部分心脏照射后用双能量microCT,4D-microCT和microspECT成像评估小鼠心脏损伤。

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摘要

PURPOSE: To develop a mouse model of cardiac injury after partial heart irradiation (PHI) and to test whether dual energy (DE)-microCT and 4-dimensional (4D)-microCT can be used to assess cardiac injury after PHI to complement myocardial perfusion imaging using micro-single photon emission computed tomography (SPECT). METHODS AND MATERIALS: To study cardiac injury from tangent field irradiation in mice, we used a small-field biological irradiator to deliver a single dose of 12 Gy x-rays to approximately one-third of the left ventricle (LV) of Tie2Cre; p53(FL/+) and Tie2Cre; p53(FL/-) mice, where 1 or both alleles of p53 are deleted in endothelial cells. Four and 8 weeks after irradiation, mice were injected with gold and iodinated nanoparticle-based contrast agents, and imaged with DE-microCT and 4D-microCT to evaluate myocardial vascular permeability and cardiac function, respectively. Additionally, the same mice were imaged with microSPECT to assess myocardial perfusion. RESULTS: After PHI with tangent fields, DE-microCT scans showed a time-dependent increase in accumulation of gold nanoparticles (AuNp) in the myocardium of Tie2Cre; p53(FL/-) mice. In Tie2Cre; p53(FL/-) mice, extravasation of AuNp was observed within the irradiated LV, whereas in the myocardium of Tie2Cre; p53(FL/+) mice, AuNp were restricted to blood vessels. In addition, data from DE-microCT and microSPECT showed a linear correlation (R(2) = 0.97) between the fraction of the LV that accumulated AuNp and the fraction of LV with a perfusion defect. Furthermore, 4D-microCT scans demonstrated that PHI caused a markedly decreased ejection fraction, and higher end-diastolic and end-systolic volumes, to develop in Tie2Cre; p53(FL/-) mice, which were associated with compensatory cardiac hypertrophy of the heart that was not irradiated. CONCLUSIONS: Our results show that DE-microCT and 4D-microCT with nanoparticle-based contrast agents are novel imaging approaches complementary to microSPECT for noninvasive assessment of the change in myocardial vascular permeability and cardiac function of mice in whom myocardial injury develops after PHI.
机译:目的:建立部分心脏照射(PHI)后的小鼠心脏损伤模型,并测试是否可以使用双能(DE)-microCT和4维(4D)-microCT评估PHI后的心脏损伤以补充心肌灌注使用微单光子发射计算机断层扫描(SPECT)进行成像。方法和材料:为了研究切线场照射对小鼠的心脏损伤,我们使用小视野生物照射器向Tie2Cre左心室(LV)的大约三分之一提供单剂量的12 Gy X射线。 p53(FL / +)和Tie2Cre; p53(FL /-)小鼠,其中p53的1个或两个等位基因在内皮细胞中缺失。辐照后第4和第8周,给小鼠注射金和碘化的基于纳米粒子的造影剂,并分别用DE-microCT和4D-microCT成像,以评估心肌血管通透性和心功能。此外,相同的小鼠用microSPECT成像以评估心肌灌注。结果:在PHI具有切线场之后,DE-microCT扫描显示Tie2Cre心肌中金纳米颗粒(AuNp)的积累随时间的增加。 p53(FL /-)小鼠。在Tie2Cre中;在p53(FL /-)小鼠中,在被照射的LV内观察到AuNp的外渗,而在Tie2Cre的心肌中观察到了。 p53(FL / +)小鼠,AuNp仅限于血管。此外,来自DE-microCT和microSPECT的数据显示,累积AuNp的LV分数与具有灌注缺陷的LV分数之间存在线性相关性(R(2)= 0.97)。此外,4D-microCT扫描显示,在Tie2Cre中,PHI导致射血分数显着降低,并且舒张末期和收缩末期容积增加。 p53(FL /-)小鼠,与未受辐照的心脏代偿性心脏肥大有关。结论:我们的结果表明,DE-microCT和4D-microCT与基于纳米粒子的造影剂是与microSPECT互补的新型成像方法,可用于无创评估PHI后发生心肌损伤的小鼠的心肌血管通透性和心脏功能的变化。

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