Identification and<i>in vivo</i>evaluation of a fluorine-18 rolipram analogue, [<sup>18</sup>F]MNI-617, as a radioligand for PDE4 imaging in mammalian brain

Thomae, David; Morley, Thomas J.; Lee, Hsiaoju; Barret, Olivier; Constantinescu, Cristian; Papin, Caroline; Baldwin, Ronald M.; Tamagnan, Gilles; Alagille, David

doi:10.1002/jlcr.3389

Cited by 10 publications

(14 citation statements)

References 37 publications

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“…Very recently, Thomae et al [82,83] reported on the development of structurally modified derivatives of ( R )- 6 with the aim to generate 18 F- and 123 I-labeled PDE4 radioligands for PET or SPECT application, respectively. In general, low tolerance of PDE4 for structural changes in ( R )- 6 has been stated as well as a significant decrease in PDE4 affinity for the iodo derivatives that consequently have been suggested to be not suitable as SPECT radioligands.…”

Section: Pde4 Radioligandsmentioning

confidence: 99%

“…In general, low tolerance of PDE4 for structural changes in ( R )- 6 has been stated as well as a significant decrease in PDE4 affinity for the iodo derivatives that consequently have been suggested to be not suitable as SPECT radioligands. Out of this series, the fluorinated analogue 7 (MNI-617, Figure 2) has been described as the most promising compound with a five-fold increased PDE4 affinity over ( R )- 6 ( K D = 0.26 nM vs. 1.6 nM) and thus has been selected for 18 F-labeling [82,83].…”

Section: Pde4 Radioligandsmentioning

confidence: 99%

“…Initially, [ 18 F] 7 has been prepared in an one-pot two-step radiosynthesis procedure via 18 F-labeling of diiodomethane using K + /[ 18 F]F − /K 2.2.2 -carbonate complex followed by O -alkylation of the corresponding phenol precursor with the resulting [ 18 F]fluoroiodomethane [82]. At the 21st International Symposium on Radiopharmaceutical Sciences, Columbia 2015, the group has presented an optimized two-step radiolabeling strategy by first generating [ 18 F]fluoromethane tosylate that has been used as a prosthetic group for subsequent O -alkylation of the phenol precursor under basic conditions (Scheme 4).…”

Section: Pde4 Radioligandsmentioning

confidence: 99%

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Novel Radioligands for Cyclic Nucleotide Phosphodiesterase Imaging with Positron Emission Tomography: An Update on Developments Since 2012

et al. 2016

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Cyclic nucleotide phosphodiesterases (PDEs) are a class of intracellular enzymes that inactivate the secondary messenger molecules, cyclic adenosine monophosphate (cAMP) and cyclic guanosine monophosphate (cGMP). Thus, PDEs regulate the signaling cascades mediated by these cyclic nucleotides and affect fundamental intracellular processes. Pharmacological inhibition of PDE activity is a promising strategy for treatment of several diseases. However, the role of the different PDEs in related pathologies is not completely clarified yet. PDE-specific radioligands enable non-invasive visualization and quantification of these enzymes by positron emission tomography (PET) in vivo and provide an important translational tool for elucidation of the relationship between altered expression of PDEs and pathophysiological effects as well as (pre-)clinical evaluation of novel PDE inhibitors developed as therapeutics. Herein we present an overview of novel PDE radioligands for PET published since 2012.

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Section: Pde4 Radioligandsmentioning

confidence: 99%

Section: Pde4 Radioligandsmentioning

confidence: 99%

Section: Pde4 Radioligandsmentioning

confidence: 99%

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Novel Radioligands for Cyclic Nucleotide Phosphodiesterase Imaging with Positron Emission Tomography: An Update on Developments Since 2012

et al. 2016

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“…Radiochemical yields are comparable and range from 60 to 80% for the final alkylation step. 37,52,53 Analogous to the O-alkylation, aromatic S-alkylation of guanidine derivative 18 has been performed (Scheme 10). The reaction was carried out in MeCN at 110 1C for 15 minutes using cesium carbonate as base.…”

Section: [ 18 F]fluoromethyl Halides and Sulfonatesmentioning

confidence: 99%

“…Reactions with [ 18 F]fluoromethyl tosylate. Scheme 9 O-Alkylated tracers with [ 18 F]fluoromethyl tosylate 37,52,53. Scheme 10 Synthesis of a S-fluoroalkyl guanidine derivative 54.…”

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confidence: 99%

Fluorine-18 labelled building blocks for PET tracer synthesis

et al. 2017

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Positron emission tomography (PET) is an important driver for present day healthcare. Fluorine-18 is the most widely used radioisotope for PET imaging and a thorough overview of the available radiochemistry methodology is a prerequisite for selection of a synthetic approach for new fluorine-18 labelled PET tracers. These PET tracers can be synthesised either by late-stage radiofluorination, introducing fluorine-18 in the last step of the synthesis, or by a building block approach (also called modular build-up approach), introducing fluorine-18 in a fast and efficient manner in a building block, which is reacted further in one or multiple reaction steps to form the PET tracer. This review presents a comprehensive overview of the synthesis and application of fluorine-18 labelled building blocks since 2010.

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Molecular Structure and Crystal Packing of Monofluoromethoxyarenes

et al. 2018

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X‐ray crystal structures of monofluoromethoxy aryl compounds are presented for the first time. In fluoromethoxybenzene derivatives with at least one unsubstituted ortho‐position, the fluoromethoxy group adopts a twisted anisole conformation. The twist is most pronounced in derivatives with the least electron‐demanding phenyl unit. The observed structural features in the crystalline state are in good agreement with theoretical predictions for prototypical monofluoromethoxybenzene. In contrast, a 5‐fluoromethoxyindole derivative exhibits a conformation differing from that by theoretical predictions. Such a difference may be due to crystal packing, in which the fluorine atom is trapped in a hydrophobic pocket lined with aliphatic C–H bonds. The crystal structures of the simple α‐monofluorinated anisoles exhibit a variety of linear and cyclic interaction motifs for the monofluoromethoxy group. Similar motifs are also observed in the crystals of other monofluoromethyl‐containing compounds. In all these crystal structures the geometrical characteristics of mutual close contacts between monofluoromethoxy or between monofluoromethyl units are dependent on their surrounding environment in the crystal structure, an observation consistent with relatively weak interactions. A survey of all close C–F···H–C contacts in these crystals and in crystal structures of CH2F‐containing compounds from the CSD reveals little evidence for significant H‐bonding character in these interactions.

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Identification andin vivoevaluation of a fluorine-18 rolipram analogue, [¹⁸F]MNI-617, as a radioligand for PDE4 imaging in mammalian brain

Cited by 10 publications

References 37 publications

Novel Radioligands for Cyclic Nucleotide Phosphodiesterase Imaging with Positron Emission Tomography: An Update on Developments Since 2012

Novel Radioligands for Cyclic Nucleotide Phosphodiesterase Imaging with Positron Emission Tomography: An Update on Developments Since 2012

Fluorine-18 labelled building blocks for PET tracer synthesis

Molecular Structure and Crystal Packing of Monofluoromethoxyarenes

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Identification andin vivoevaluation of a fluorine-18 rolipram analogue, [18F]MNI-617, as a radioligand for PDE4 imaging in mammalian brain

Cited by 10 publications

References 37 publications

Novel Radioligands for Cyclic Nucleotide Phosphodiesterase Imaging with Positron Emission Tomography: An Update on Developments Since 2012

Novel Radioligands for Cyclic Nucleotide Phosphodiesterase Imaging with Positron Emission Tomography: An Update on Developments Since 2012

Fluorine-18 labelled building blocks for PET tracer synthesis

Molecular Structure and Crystal Packing of Monofluoromethoxyarenes

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Identification andin vivoevaluation of a fluorine-18 rolipram analogue, [¹⁸F]MNI-617, as a radioligand for PDE4 imaging in mammalian brain