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Drug-induced cardiomyopathy:Characterization of a rat model by^18 FFDG/PET and^99m TcMIBI/SPECT

机译:药物诱导的心肌病:通过^ 18 f FDG / PET和^ 99M TC MIBI / SPECT的大鼠模型的表征

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Background:Drug-induced cardiomyopathy is a significant medical problem.Clinical diagnosis of myocardial injury is based on initial electrocardiogram,levels of circulating biomarkers,and perfusion imaging with single photon emission computed tomography(SPECT).Positron emission tomography(PET)is an alternative imaging modality that provides better resolution and sensitivity than SPECT,improves diagnostic accuracy,and allows therapeutic monitoring.The objective of this study was to assess the detection of drug-induced cardiomyopathy by PET using 2-deoxy-2-[^18F]fluoro-D-glucose(FDG)and compare it with the conventional SPECT technique with[^99m Tc]-Sestamibi(MIBI).Methods:Cardiomyopathy was induced in Sprague Dawley rats using high-dose isoproterenol.Nuclear[^18F]FDG/PET and[^99m Tc]MIBI/SPECT were performed before and after isoproterenol administration.[^18F]FDG(0.1 mCi,200-400μL)and[^99m Tc]MIBI(2 mCi,200-600μL)were administered via the tail vein and imaging was performed 1 hour postinjection.Isoproterenol-induced injury was confirmed by the plasma level of cardiac troponin and triphenyltetrazolium chloride(TTC)staining.Results:Isoproterenol administration resulted in an increase in circulating cardiac troponin I and showed histologic damage in the myocardium.Visually,preisoproterenol and postisoproterenol images showed alterations in cardiac accumulation of[^18F]FDG,but not of[^99m Tc]MIBI.Image analysis revealed that myocardial uptake of[^18F]FDG reduced by 60%after isoproterenol treatment,whereas that of[^99m Tc]MIBI decreased by 45%.Conclusion:We conclude that[^18F]FDG is a more sensitive radiotracer than[^99m Tc]MIBI for imaging of drug-induced cardiomyopathy.We theorize that isoproterenolinduced cardiomyopathy impacts cellular metabolism more than perfusion,which results in more substantial changes in[^18F]FDG uptake than in[^99m Tc]MIBI accumulation in cardiac tissue.
机译:背景:药物诱导的心肌病是一种重要的医学问题。心肌损伤的临床诊断是基于初始心电图,循环生物标志物的水平,以及用单光子发射计算断层摄影(SPECT).Postron发射断层扫描(PET)的灌注成像是一种替代提供比SPECT的更好分辨率和灵敏度的成像模型提高了诊断准确性,并允许治疗性监测。本研究的目的是使用2-DEOXY-2 - [18F] Fluoro评估PET的药物诱导心肌病的检测D-葡萄糖(FDG)并将其与常规的SPECT技术与[^ 99M TC] -Sestamibi(MIBI)进行比较。方法:使用高剂量异丙肾上腺素诱导心肌病,在Sprague Dawley大鼠中诱导。核[18F] FDG / PET和在异丙烯酚给药前后进行MIBI / SPECT。通过尾静脉(2mCI,200-400μl)和[^ 99m,200-600μl]和[^ 99M,200-600μl]进行FDG(0.1MCI,200-400μL)和成像进行1小时Postinj Encent.Sepoterenol诱导的损伤是通过心肌肌钙蛋白和三苯基四唑氯(TTC)染色的血浆水平证实。结果:异丙肾上腺酮导致循环心肌肌钙蛋白I的增加,并在心肌中显示组织学损伤。,前,前蛋白醇和多蛋白酶图像表现出[^ 18F] FDG的心脏积累的改变,但不是[^ 99m Tc] mibi.imimi.Imimard分析表明,异丙酚处理后[^ 18F] FDG的心肌摄取减少了60%,而[^ 99M TC] MIBI减少了45%。结论:我们得出结论,FDG是一种比[99M TC] MIBI更敏感的放射性机器,用于对药物诱导的心肌病成像进行成像。我们大化了异丙灭绝的心肌病影响细胞代谢比灌注更多,这是在效率更大于FDG摄取而不是心脏组织中的[^ 99M TC] MIBI积累。

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