Fast indirect fluorine-18 labeling of protein/peptide using the useful 6-fluoronicotinic acid-2,3,5,6-tetrafluorophenyl prosthetic group: A method comparable to direct fluorination

Basuli, Falguni; Zhang, Xiang; Woodroofe, Carolyn C.; Jagoda, Elaine M.; Choyke, Peter L.; Swenson, Rolf E.

doi:10.1002/jlcr.3487

Cited by 24 publications

(32 citation statements)

References 66 publications

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“…We wanted to test the [ 18 F] fluoride elution efficiency using a quaternary ammonium triflate precursor (Scheme 1, 1) of benzaldehyde in different solvents with the intention to directly incorporate the fluoride in the product. Attempts to elute [ 18 F]fluoride from the Sep-Pak with 1 in acetonitrile were unsuccessful (Table 1) ammonium triflate precursor (2) in acetonitrile through the Sep-Pak containing [ 18 F]fluoride. Fluoride elution efficiency was tested using different conditions ( Table 1).…”

Section: Resultsmentioning

confidence: 99%

Rapid synthesis of maleimide functionalized fluorine‐18 labeled prosthetic group using “radio‐fluorination on the Sep‐Pak” method

Basuli

Zhang

Jagoda

et al. 2018

Labelled Comp Radiopharmac

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Following our recently published fluorine-18 labeling method, "Radio-fluorination on the Sep-Pak", we have successfully synthesized 6-[ F]fluoronicotinaldehyde by passing a solution (1:4 acetonitrile: t-butanol) of its quaternary ammonium salt precursor, 6-(N,N,N-trimethylamino)nicotinaldehyde trifluoromethanesulfonate (2), through a fluorine-18 containing anion exchange cartridge (PS-HCO ). Over 80% radiochemical conversion was observed using 10 mg of precursor within 1 minute. The [ F]fluoronicotinaldehyde ([ F]5) was then conjugated with 1-(6-(aminooxy)hexyl)-1H-pyrrole-2,5-dione to prepare the fluorine-18 labeled maleimide functionalized prosthetic group, 6-[ F]fluoronicotinaldehyde O-(6-(2,5-dioxo-2,5-dihydro-1H-pyrrol-1-yl)hexyl) oxime, 6-[ F]FPyMHO ([ F]6). The current Sep-Pak method not only improves the overall radiochemical yield (50 ± 9%, decay-corrected, n = 9) but also significantly reduces the synthesis time (from 60-90 minutes to 30 minutes) when compared with literature methods for the synthesis of similar prosthetic groups.

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Section: Resultsmentioning

confidence: 99%

Rapid synthesis of maleimide functionalized fluorine‐18 labeled prosthetic group using “radio‐fluorination on the Sep‐Pak” method

Basuli

Zhang

Jagoda

et al. 2018

Labelled Comp Radiopharmac

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“…38,[44][45][46] Although Olberg, Malik, and others have demonstrated the effectiveness of the [ 18 F]FPy-TFP prosthetic group for radiolabelling various peptides, intermediate purication of the [ 18 F]FPy-TFP was required prior to conjugation to a peptide in order to remove unreacted PyTFP-precursor that interferes with peptide radiolabeling. 38,[44][45][46] In addition, Olberg et al showed that hydrolysis of the PyTFP-precursor resulted in formation of 2,3,5,6-tetrauorophenyl-6-(2,3,5,6-tetrauorophenoxy)nicotinate (by-product (11)), which can hinder efficient radiolabeling of the peptide. 38 To facilitate purication, the ELIXYS FLEX/CHEM® radiosynthesizer can accommodate SPE-cartridges in multiple congurations, enabling intermediate cartridge based purications within the reaction sequence.…”

Section: Discussionmentioning

confidence: 99%

“…These yields are comparable to other automated 18 32 Radiolabeling of peptides with [ 18 F]FPy-TFP were previously performed manually using a variety of peptide coupling conditions. 38,[44][45][46] The original manual peptide radiolabeling with [ 18 F]FPy-TFP by Olberg et al utilized a 1 : 1 : 1 DMSO : MeCN : phosphate buffer (pH-9.0), 3-5 mg of peptide, and a reaction temperature of 40 C for 15 minutes to generate the [ 18 F]FPy-peptide in a 22.5 AE 6.0% yield (total synthesis time ¼ 85 minutes). 38 Malik et al manually radiolabeled a DUPApeptide (2 mg) with [ 18 F]FPy-TFP in 5 : 3 MeCN : H 2 O, containing 5.5 mg of sodium bicarbonate as a base, at 60 C for 10 minutes, resulting in a 48 AE 0.9% non-decay corrected yield (total synthesis time ¼ 50 minutes).…”

Section: Discussionmentioning

confidence: 99%

Fully automated peptide radiolabeling from [¹⁸F]fluoride

et al. 2019

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The biological properties of receptor-targeted peptides have made them popular diagnostic imaging and therapeutic agents. Typically, the synthesis of fluorine-18 radiolabeled receptor-targeted peptides for positron emission tomography (PET) imaging is a time consuming, complex, multi-step synthetic process that is highly variable based on the peptide. The complexity associated with the radiolabeling route and lack of robust automated protocols can hinder translation into the clinic. A fully automated batch production to radiolabel three peptides (YGGFL, cRGDyK, and Pyr-QKLGNQWAVGHLM) from fluorine-18 using the ELIXYS FLEX/CHEM® radiosynthesizer in a two-step process is described. First, the prosthetic group, 6-[ 18 F]fluoronicotinyl-2,3,5,6-tetrafluorophenyl ester ([ 18 F]FPy-TFP) was synthesized and subsequently attached to the peptide. The [ 18 F]FPy-peptides were synthesized in 13-26% decay corrected yields from fluorine-18 with high molar activity 1-5 Ci mmol À1 and radiochemical purity of >99% in an overall synthesis time of 97 AE 3 minutes.

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“…It is noteworthy that the [18 F]F-Py-TFP prosthetic group can be prepared in one step from the trimethylammonium precursor [46] and it has been utilized in the fluorine-18 labeling of albumin and c(RGDfK). [47] …”

Section: Indirect Methods For 18f-radiolabeling Of Biomoleculesmentioning

confidence: 99%

¹⁸F‐Labeling of Sensitive Biomolecules for Positron Emission Tomography

Krishnan

Vasdev

et al. 2017

Chemistry A European J

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Positron emission tomography (PET) imaging study of fluorine-18 labeled biomolecules is an emerging and rapidly growing area for preclinical and clinical research. The present review focuses on recent advances in radiochemical methods for incorporating fluorine-18 into biomolecules via ‘direct’ or ‘indirect’ bioconjugation. Recently developed prosthetic groups and pre-targeting strategies, as well as representative examples in 18F-labeling of biomolecules in PET imaging research studies are highlighted.

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Fast indirect fluorine-18 labeling of protein/peptide using the useful 6-fluoronicotinic acid-2,3,5,6-tetrafluorophenyl prosthetic group: A method comparable to direct fluorination

Cited by 24 publications

References 66 publications

Rapid synthesis of maleimide functionalized fluorine‐18 labeled prosthetic group using “radio‐fluorination on the Sep‐Pak” method

Rapid synthesis of maleimide functionalized fluorine‐18 labeled prosthetic group using “radio‐fluorination on the Sep‐Pak” method

Fully automated peptide radiolabeling from [¹⁸F]fluoride

¹⁸F‐Labeling of Sensitive Biomolecules for Positron Emission Tomography

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Fast indirect fluorine-18 labeling of protein/peptide using the useful 6-fluoronicotinic acid-2,3,5,6-tetrafluorophenyl prosthetic group: A method comparable to direct fluorination

Cited by 24 publications

References 66 publications

Rapid synthesis of maleimide functionalized fluorine‐18 labeled prosthetic group using “radio‐fluorination on the Sep‐Pak” method

Rapid synthesis of maleimide functionalized fluorine‐18 labeled prosthetic group using “radio‐fluorination on the Sep‐Pak” method

Fully automated peptide radiolabeling from [18F]fluoride

18F‐Labeling of Sensitive Biomolecules for Positron Emission Tomography

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Fully automated peptide radiolabeling from [¹⁸F]fluoride

¹⁸F‐Labeling of Sensitive Biomolecules for Positron Emission Tomography