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首页> 外文期刊>Journal of Medicinal Chemistry >Development of 2-Deoxy-2-[F-18]fluororibose for Positron Emission Tomography Imaging Liver Function in Vivo
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Development of 2-Deoxy-2-[F-18]fluororibose for Positron Emission Tomography Imaging Liver Function in Vivo

机译:用于正电子发射断层扫描成像体内肝功能的2-脱氧-2- [F-18]氟核糖的开发

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Life-threatening: acute liver failure can be triggered, by a variety of factors,, including common drugs such as acetaminophen,. Positron emission tomography (BET) is rarely used to monitor liver function, In part because of a lack of specific imaging agents for liver function.. Here we report a new PET probe, 2-deoxy-2[F-18]fluororibose ([F-18]-2-DFR), for use in imaging liver function. [F-18]-2-DFR was synthesized and validated as a competitive substrate for the ribose salvage pathway. [F-18]-2-DFR was prepared through an efficient late Stage radiofluorination. The desired selectivity of fluorination was achieved using an unorthodox protecting group on the precursor, which could withstand harsh S(N)2 reaction conditions with no side reactions.[F-18,]-2-DFR accumulated preferentially in the liver and was metabolized by the same enzymes, as ribose. [F-18]-2-DFR could distinguish between healthy liver and, liver damaged by acetaminophen. [(18)]-2-DFR is expected to-be a useful PET probe for imaging and quantifying liver functions in vivo, with likely significant clinical utility.
机译:威胁生命的:可由多种因素触发急性肝衰竭,包括对乙酰氨基酚等常见药物。正电子发射断层扫描(BET)很少用于监测肝功能,部分原因是缺乏用于肝功能的特异性成像剂。在这里,我们报道一种新的PET探针2-deoxy-2 [F-18]氟核糖([ F-18] -2-DFR),用于肝功能成像。合成了[F-18] -2-DFR,并证实其可作为核糖挽救途径的竞争底物。 [F-18] -2-DFR是通过高效的后期放射性氟化制备的。在前体上使用非传统的保护基即可达到所需的氟化选择性,该保护基可承受苛刻的S(N)2反应条件,而无副反应。[F-18,]-2-DFR优先在肝脏中积累并代谢。通过与核糖相同的酶[F-18] -2-DFR可以区分健康的肝脏和对乙酰氨基酚损伤的肝脏。 [(18)]-2-DFR有望成为一种有用的PET探针,用于体内成像和定量肝功能,可能具有重要的临床应用价值。

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