Literature DB >> 28826521

Exploring Metabolism In Vivo Using Endogenous 11C Metabolic Tracers.

Kiel Neumann1, Robert Flavell1, David M Wilson2.   

Abstract

Cancer and other diseases are increasingly understood in terms of their metabolic disturbances. This thinking has revolutionized the field of ex vivo metabolomics and motivated new approaches to detect metabolites in living systems, including proton magnetic resonance spectroscopy (1H-MRS), hyperpolarized 13C MRS, and PET. For PET, imaging abnormal metabolism in vivo is hardly new. Positron-labeled small-molecule metabolites have been used for decades in humans, including 18F-FDG, which is used frequently to detect upregulated glycolysis in tumors. Many current 18F metabolic tracers including 18F-FDG have evolved from their 11C counterparts, chemically identical to endogenous substrates and thus approximating intrinsic biochemical pathways. This mimicry has stimulated the development of new radiochemical methods to incorporate 11C and inspired the synthesis of a large number of 11C endogenous radiotracers. This is in spite of the 20-minute half-life of 11C, which generally limits its use in patients to centers with an on-site cyclotron. Innovation in 11C chemistry has persisted in the face of this limitation, because (1) the radiochemists involved are inspired, (2) the methods of 11C incorporation are diverse, and (3) 11C compounds often show more predictable in vivo behavior, thus representing an important first step in the validation of new tracer concepts. In this mini-review we will discuss some of the general motivations behind PET tracers, rationales for the use of 11C, and some of the special challenges encountered in the synthesis of 11C endogenous compounds. Most importantly, we will try to highlight the exceptional creativity used in early 11C tracer syntheses, which used enzyme-catalyzed and other "green" methods before these concepts were commonplace.
Copyright © 2017. Published by Elsevier Inc.

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Year:  2017        PMID: 28826521      PMCID: PMC6037183          DOI: 10.1053/j.semnuclmed.2017.05.003

Source DB:  PubMed          Journal:  Semin Nucl Med        ISSN: 0001-2998            Impact factor:   4.446


  72 in total

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Authors:  J Scott Brockenbrough; Timothee Souquet; Janice K Morihara; Joshua E Stern; Stephen E Hawes; Janet S Rasey; Antoine Leblond; Linda W Wiens; Qinghua Feng; John Grierson; Hubert Vesselle
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5.  Synthesis and evaluation of 18F-labeled choline as an oncologic tracer for positron emission tomography: initial findings in prostate cancer.

Authors:  T R DeGrado; R E Coleman; S Wang; S W Baldwin; M D Orr; C N Robertson; T J Polascik; D T Price
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6.  Tau Positron Emission Tomography (PET) Imaging: Past, Present, and Future.

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7.  Preparation and characterization of L-[5-11C]-glutamine for metabolic imaging of tumors.

Authors:  Wenchao Qu; Shunichi Oya; Brian P Lieberman; Karl Ploessl; Limin Wang; David R Wise; Chaitanya R Divgi; Lewis A Chodosh; Lewis P Chodosh; Craig B Thompson; Hank F Kung
Journal:  J Nucl Med       Date:  2011-12-15       Impact factor: 10.057

8.  Regional brain kinetics of 6-fluoro-(beta-11C)-L-dopa and (beta-11C)-L-dopa following COMT inhibition. A study in vivo using positron emission tomography.

Authors:  P Hartvig; K J Lindner; J Tedroff; P Bjurling; K Hörnfelt; B Långström
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9.  Synthesis of L- and D-[methyl-11C]methionine.

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Review 10.  Characteristics of Tau and Its Ligands in PET Imaging.

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Review 2.  Nuclear Imaging of Glucose Metabolism: Beyond 18F-FDG.

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  3 in total

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