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Characterization and predictive value of near infrared 2-deoxyglucose optical imaging in severe acute pancreatitis

机译:重症急性胰腺炎的近红外光2-脱氧葡萄糖光学成像的表征及预测价值

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摘要

© 2016 de Oliveira et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Background: Studying the uptake of 2-deoxy glucose (2-DG) analogs such as 2-Deoxy-2-[18F] fluoroglucose (FDG) is a common approach to identify and monitor malignancies and more recently chronic inflammation. While pancreatitis is a common cause for false positive results in human studies on pancreatic cancer using FDG, the relevance of these findings to acute pancreatitis (AP) is unknown. FDG has a short half-life. Thus, with an aim to accurately characterize the metabolic demand of the pancreas during AP in real-time, we studied the uptake of the non-radioactive, near infrared fluorescence labelled 2-deoxyglucose analog, IRDye1 ® 800CW 2-DG probe (NIR 2-DG; Li-Cor) during mild and severe biliary AP. Methods: Wistar rats (300 g; 8-12/group) were administered NIR 2-DG (10 nM; I.V.). Mild and severe biliary AP were respectively induced by biliopancreatic d uct ligation (DL) alone or along with infusing glyceryl trilinoleate (GTL; 50 μL/100 g) within 10 minutes of giving NIR 2-DG. Controls (CON) only received NIR 2-DG. Imaging was done every 5-10 minutes over 3 hrs. Average Radiant Efficiency [p/s/cm 2 /sr]/[μW/cm 2 ] was measured over the pancreas using the IVIS 200 in-vivo imaging system (PerkinElmer) using the Living Image ® software and verified in ex vivo pancreata. Blood amylase, lipase and pancreatic edema, necrosis were measured over the course of AP. Results: NIR 2-DG uptake over the first hour was not influenced by AP induction. However, while the signal declined in controls and rats with mild AP, there was significantly higher retention of NIR 2-DG in the pancreas after 1 hour in those with GTL pancreatitis. The increase was > 3 fold over controls in the GTL group and was verified to be in the pancreas ex vivo. In vitro, pancreatic acini exposed to GTL had a similar increase in NIR 2-DG uptake which was followed by progressively worse acinar necrosis. Greater retention of NIR 2-DG in vivo was associated with worse pancreatic necrosis, reduced ATP concentrations and mortality, which were not predicted by the blood parameters. Conclusion: In-vivo fluorescent imaging of a non-radioactive near infrared 2-DG optical probe can predict the AP severity early during the disease.
机译:©2016 de Oliveira等。这是根据知识共享署名许可协议的条款分发的开放获取文章,该条款允许在任何媒介中无限制地使用,分发和复制,但要注明原始作者和出处。背景:研究2-脱氧葡萄糖(2-DG)类似物(例如2-脱氧-2- [18F]氟葡萄糖(FDG))的摄取是识别和监测恶性肿瘤以及最近发生的慢性炎症的常见方法。尽管胰腺炎是人类使用FDG研究胰腺癌的假阳性结果的常见原因,但这些发现与急性胰腺炎(AP)的相关性尚不清楚。 FDG的半衰期短。因此,为了实时准确表征AP期间胰腺的代谢需求,我们研究了非放射性,近红外荧光标记的2-脱氧葡萄糖类似物IRDye1®800CW 2-DG探针(NIR 2)的摄取。 -DG; Li-Cor)在轻度和重度胆道AP期间。方法:Wistar大鼠(300 g,8-12只/组)接受NIR 2-DG(10 nM; I.V.)。在给予NIR 2-DG的10分钟内,仅通过胆管胰结扎术(DL)或与甘油三亚油酸酯(GTL; 50μL/ 100 g)一起输注分别诱导了轻度和重度胆汁性AP。控件(CON)仅收到NIR 2-DG。在3小时内每5-10分钟进行一次成像。使用IVIS 200体内成像系统(PerkinElmer),使用LivingImage®软件在胰腺上测量平均辐射效率[p / s / cm 2 / sr] / [μW/ cm 2],并在离体胰腺中进行验证。在AP的过程中测量了血液淀粉酶,脂肪酶和胰腺水肿,坏死。结果:第一个小时的NIR 2-DG吸收不受AP诱导的影响。然而,尽管在轻度AP的对照组和大鼠中信号减弱,但是在GTL胰腺炎患者中,在1小时后,胰腺中NIR 2-DG的保留明显更高。 GTL组的增加超过对照的3倍,并且被证实是胰腺离体的。在体外,暴露于GTL的胰腺腺泡在NIR 2-DG摄取方面有相似的增加,随后腺泡坏死逐渐恶化。 NIR 2-DG在体内的保留更大,与胰腺坏死恶化,ATP浓度降低和死亡率降低有关,而血液参数并未预测到这种情况。结论:非放射性近红外2-DG光学探针的体内荧光成像可以预测疾病早期的AP严重程度。

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