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首页> 外文期刊>Nuclear Medicine and Biology >Comparison of radiolabeled isatin analogs for imaging apoptosis with positron emission tomography.
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Comparison of radiolabeled isatin analogs for imaging apoptosis with positron emission tomography.

机译:用正电子发射断层显像对放射性标记的类似素进行细胞凋亡成像的比较。

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INTRODUCTION: Caspase-3 is one of the executioner caspases activated as a result of apoptosis. Radiolabeled isatins bind to caspase-3 with high affinity and are potential tracers for use with positron emission tomography to image apoptosis. We compared the ability of two novel radiolabeled isatins, [18F]WC-IV-3 and [11C]WC-98, to detect caspase-3 activation in a rat model of cycloheximide-induced liver injury. METHODS: Male Sprague-Dawley rats were treated with cycloheximide and then imaged with microPET 3 h later with [18F]WC-IV-3 and [11C]WC-98. Biodistribution studies were also performed simultaneously, with caspase-3 activation verified by fluorometric enzyme assay and Western blots. RESULTS: MicroPET imaging studies demonstrated similar behavior of both tracers but with a lower maximum peak with [11C]WC-98 than with [18F]WC-IV-3. Biodistribution studies demonstrated increased uptake of both tracers in the liver and spleen, but this was statistically significant only in the liver with both compounds. The level of [18F]WC-IV-3 uptake appeared to correlate roughly with rates of caspase-3 activation by the enzyme assay, but the magnitude of difference between treated and control groups was lower than that observed in previously published data with [18F]WC-II-89, another radiolabeled isatin analog. Activation was also confirmed in the liver and spleen but not in fat by Western blot. CONCLUSION: [18F]WC-IV-3 uptake appears to correlate with increased caspase-3 enzyme activity, but the dynamic range of uptake of these two tracers appears to be less than that seen with [18F]WC-II-89. Studies are ongoing to verify these results in other animal models of apoptosis.
机译:简介:Caspase-3是因凋亡而激活的the子执行酶之一。放射性标记的isatins以高亲和力与caspase-3结合,并且是潜在的示踪剂,可与正电子发射断层扫描一起使用来对细胞凋亡进行成像。我们比较了两种新型放射性标记的靛红[18F] WC-IV-3和[11C] WC-98在环己酰亚胺诱发的肝损伤大鼠模型中检测caspase-3活化的能力。方法:雄性Sprague-Dawley大鼠用环己酰亚胺治疗,然后在3 h后用[18F] WC-IV-3和[11C] WC-98用microPET成像。生物分布研究也同时进行,caspase-3激活通过荧光酶测定和Western印迹验证。结果:MicroPET成像研究表明两种示踪剂的行为相似,但是[11C] WC-98的最大峰比[18F] WC-IV-3的低。生物分布研究表明,肝脏和脾脏中两种示踪剂的摄取均增加,但这仅在两种化合物中均具有统计学意义。 [18F] WC-IV-3的摄取水平似乎与酶测定法中的caspase-3活化率大致相关,但是治疗组和对照组之间的差异幅度低于先前发表的[18F]数据中观察到的差异。 ] WC-II-89,另一种放射性标记的类似素。还通过Western印迹证实了在肝和脾中的活化,但在脂肪中没有活化。结论:[18F] WC-IV-3的摄取似乎与caspase-3酶活性的增加有关,但是这两种示踪剂的摄取动态范围似乎小于[18F] WC-II-89。正在进行研究以在其他细胞凋亡动物模型中验证这些结果。

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