Evaluation of [<sup>11</sup>C]<i>N</i>-Methyl Lansoprazole as a Radiopharmaceutical for PET Imaging of Tau Neurofibrillary Tangles

Shao, Xia; Carpenter, Garrett; Desmond, Timothy J.; Sherman, Phillip; Quesada, Carole; Fawaz, Maria V.; Brooks, Allen F.; Kilbourn, Michael R.; Albin, Roger L.; Frey, Kirk A.; Scott, Peter J. H.

doi:10.1021/ml300216t

Cited by 52 publications

(68 citation statements)

References 32 publications

(59 reference statements)

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“…11 C-N-methyl lansoprazole is the 11 C-labeled version of the Food and Drug Administration-approved drug lansoprazole and appears to have an exceptionally high affinity for tau (8). However, to the best of our knowledge no human data have been published with this radiotracer yet.…”

Section: Overview Of Tau Pet Tracers Under Developmentmentioning

confidence: 99%

Molecular Imaging Insights into Neurodegeneration: Focus on Tau PET Radiotracers

Shah

Catafau

2014

J Nucl Med

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Neurodegenerative diseases are characterized by progressive dysfunction and neuronal death, showing specific protein inclusions at autopsy. In vivo detection of these key proteins, namely amyloid-β, tau, α-synuclein, and trans-active response DNAbinding protein 43 kDa, is possible by means of molecular neuroimaging techniques, such as PET. The development of selective PET radiotracers targeting these proteins is critical for early and accurate diagnosis and for the successful development of disease-modifying therapies. Selective PET radiotracers for amyloid-β are already available, and potential tau tracers are emerging as new-generation biomarkers. An overview of the tau-PET radiotracer development scenario, focusing on tracers that are presently being examined in humans, is presented.

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Section: Overview Of Tau Pet Tracers Under Developmentmentioning

confidence: 99%

Molecular Imaging Insights into Neurodegeneration: Focus on Tau PET Radiotracers

Shah

Catafau

2014

J Nucl Med

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“…Given that Pgp transporter expression is significantly higher in rodents than primates [26], and that we have previously seen species differences in brain uptake of radiotracers because of this [16], we chose to also evaluate [ 11 C]PyrATP-1 in rhesus macaque (n = 1). However in this case, the lack of brain uptake was found to be interspecific, and no brain uptake was apparent from the primate scan either (Figure 3c).…”

Section: Resultsmentioning

confidence: 99%

“…Dysfunction of this process is thought to generate the hyperphosphorylated tau that aggregates into tau neurofibrillary tangles in Alzheimer’s disease [6, 15], and is aligned with our program developing radiotracers for PET imaging of tau [16]. In our search for a radiotracer that would enable PET imaging of GSK-3β, we were particularly attracted by a recent report of a family of pyrazines (e.g.…”

Section: Introductionmentioning

confidence: 99%

Synthesis and evaluation of [11C]PyrATP-1, a novel radiotracer for PET imaging of glycogen synthase kinase-3β (GSK-3β)

Cole

Shao

Sherman

et al. 2014

Nuclear Medicine and Biology

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Introduction The dysfunction of glycogen synthase kinase-3β(GSK-3β) has been implicated in a number of diseases, including Alzheimer’s disease. The ability to non-invasively quantify GSK-3βactivity in vivo is therefore of critical importance, and this work is focused upon development of inhibitors of GSK-3βradiolabeled with carbon-11 to examine quantification of the enzyme using positron emission tomography (PET) imaging. Methods [11C]PyrATP-1 was prepared from the corresponding desmethyl-piperazine precursor in an automated synthesis module. In vivo rodent and primate imaging studies were conducted on a Concorde MicroPET P4 scanner to evaluate imaging properties, and in vitro autoradiography studies with rat brain samples were carried out to examine specific binding. Results 2035 ± 518 MBq (55 ± 14 mCi) of [11C]PyrATP-1 were obtained (1–2% noncorrected radiochemical yield at end-of-synthesis based upon [11C]CO2) with high chemical (>95%) and radiochemical (>99%) purities, and good specific activities (143 ± 52 GBq/µmol (3874 ± 1424 Ci/mmol)), n = 5. In vivo microPET imaging studies revealed poor brain uptake in rodents and non-human primates. Pretreatment of rodents with cyclosporin A resulted in moderately increased brain uptake suggesting Pgp transporter involvement. Autoradiography demonstrated high levels of specific binding in areas of the rodent brain known to be rich in GSK-3β. Conclusion [11C]PyrATP-1 is readily synthesized using standard carbon-11 radiochemistry. However, the poor brain uptake in rodents and non-human primates indicates that the radiotracer is not suitable for the purposes of quantifying GSK-3βin neurological and psychiatric disorders.

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“…For example, at its simplest, biodistribution studies with radiolabeled versions of drug candidates can be used to non-invasively determine whether or not a molecule reaches the target tissue in vivo in rodents and primates initially, and eventually in humans. For example, this approach can be used in the development of CNS drugs to evaluate whether or not a candidate molecule crosses the blood-brain-barrier [254]. Data obtained from such experiments can also provide a wealth of other important information, such as whether or not a drug candidate also accumulates at non-target sites with potential to cause side effects or dose-limiting toxicity at intended therapeutic doses.…”

Section: Applications Of Pet Imagingmentioning

confidence: 99%

Radiosyntheses using Fluorine-18: The Art and Science of Late Stage Fluorination

Cole¹,

Stewart²,

Littich³

et al. 2014

CTMC

123

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Positron (β+) emission tomography (PE) is a powerful, noninvasive tool for the in vivo, three-dimensional imaging of physiological structures and biochemical pathways. The continued growth of PET imaging relies on a corresponding increase in access to radiopharmaceuticals (biologically active molecules labeled with short-lived radionuclides such as fluorine-18). This unique need to incorporate the short-lived fluorine-18 atom (t1/2 = 109.77 min) as late in the synthetic pathway as possible has made development of methodologies that enable rapid and efficient late stage fluorination an area of research within its own right. In this review we describe strategies for radiolabeling with fluorine-18, including classical fluorine-18 radiochemistry and emerging techniques for late stage fluorination reactions, as well as labeling technologies such as microfluidics and solid-phase radiochemistry. The utility of fluorine-18 labeled radiopharmaceuticals is showcased through recent applications of PET imaging in the healthcare, personalized medicine and drug discovery settings.

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Evaluation of [¹¹C]N-Methyl Lansoprazole as a Radiopharmaceutical for PET Imaging of Tau Neurofibrillary Tangles

Cited by 52 publications

References 32 publications

Molecular Imaging Insights into Neurodegeneration: Focus on Tau PET Radiotracers

Molecular Imaging Insights into Neurodegeneration: Focus on Tau PET Radiotracers

Synthesis and evaluation of [11C]PyrATP-1, a novel radiotracer for PET imaging of glycogen synthase kinase-3β (GSK-3β)

Radiosyntheses using Fluorine-18: The Art and Science of Late Stage Fluorination

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Evaluation of [11C]N-Methyl Lansoprazole as a Radiopharmaceutical for PET Imaging of Tau Neurofibrillary Tangles

Cited by 52 publications

References 32 publications

Molecular Imaging Insights into Neurodegeneration: Focus on Tau PET Radiotracers

Molecular Imaging Insights into Neurodegeneration: Focus on Tau PET Radiotracers

Synthesis and evaluation of [11C]PyrATP-1, a novel radiotracer for PET imaging of glycogen synthase kinase-3β (GSK-3β)

Radiosyntheses using Fluorine-18: The Art and Science of Late Stage Fluorination

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Evaluation of [¹¹C]N-Methyl Lansoprazole as a Radiopharmaceutical for PET Imaging of Tau Neurofibrillary Tangles