-甲基-p-(123I)-碘苯五酸单光子发射计算机断层扫描在心肌病中的应用。

T Nishimura
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引用次数: 12

摘要

β -甲基-p-(123I)-碘苯五酸(BMIPP)是一种支链游离脂肪酸,具有较高的摄取率和较长的心肌滞留时间,适合心肌SPECT。本文综述了BMIPP心肌SPECT评价心肌病的最新进展。肥厚性心肌病(HCM)患者中80%存在BMIPP缺陷。此外,在肥厚区相应的部位,BMIPP的摄取减少,铊的摄取增加。BMIPP SPECT严重程度评分与室间隔壁厚度、左室功能的相关性较好,提示BMIPP更适合于HCM患者心肌完整性的评估。在扩张型心肌病(DCM)中,BMIPP与铊缺损的分离并不常见。采用BMIPP心肌SPECT评价辅酶Q10对DCM患者的治疗效果。辅酶Q10治疗后,心脏与纵隔比值和BMIPP缺损评分显著降低。BMIPP心肌SPECT从代谢显像角度评价治疗效果较为敏感。最近,在一小部分患者(0.3%-1.2%)中发现心肌摄取缺乏BMIPP。应用BMIPP和18F-FDG对ⅰ型CD36缺乏症患者进行心脏放射性核素显像。18F-FDG的剂量摄取百分比明显高于正常对照。乳糜泻是一种主要的心肌长链脂肪酸转运体,其缺失可能导致心肌葡萄糖摄取代偿性上调。在心肌病中CD36缺乏的频率增加。因此,脂肪酸转运蛋白及其与BMIPP摄取相关的基因缺陷可能成为未来的一个重要问题。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
beta-Methyl-p-(123I)-iodophenyl pentadecanoic acid single-photon emission computed tomography in cardiomyopathy.

beta-Methyl-p-(123I)-iodophenyl pentadecanoic acid (BMIPP) is one of the branched-chain free fatty acids, which has suitable characteristics for myocardial SPECT because of higher uptake and longer retention in the myocardium. Recent advances of BMIPP myocardial SPECT for evaluating cardiomyopathy were reviewed. BMIPP defects were observed in 80% patients with hypertrophic cardiomyopathy (HCM). Moreover, BMIPP uptake was reduced at sites that corresponded with hypertrophic areas, where thallium uptake was increased. The correlations between severity score and septal wall thickness and LV function were better with BMIPP SPECT, suggesting that BMIPP is more suitable for the assessment of myocardial integrity in HCM. The dissociation between BMIPP and thallium defects was not observed frequently in dilated cardiomyopathy (DCM). We carried out BMIPP myocardial SPECT to evaluate the therapeutic effects of co-enzyme Q10 on DCM patients. Hearts to the mediastinum ratio and BMIPP defect scores were significantly decreased after co-enzyme Q10 treatment. BMIPP myocardial SPECT was confirmed to be sensitive in evaluating the therapeutic effect for the perspective of metabolic SPECT imaging. Recently, a lack of myocardial uptake of BMIPP has been found in a small subset of patients (0.3%-1.2%). Cardiac radionuclide imaging using BMIPP and 18F-FDG were performed on patients with type I CD36 deficiency. The percent dose uptake of 18F-FDG was significantly higher than in normal controls. CD functions as a major myocardial long-chain fatty acid transporter and its absence may lead to a compensatory upregulation of myocardial glucose uptake. An increased frequency of CD36 deficiency was demonstrated in cardiomyopathy. Therefore, fatty acid transport proteins and their related gene defects in relation to BMIPP uptake may become an important issue in the future.

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