simplifying the preparation of 18 f-based biomolecular imaging agents through ‘click’ chemistry

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James Inkster, Msc., SFU/TRIUMF Simplifying the Preparation of 18 F- based Biomolecular Imaging Agents Through ‘Click’ Chemistry CANADA’S NATIONAL LABORATORY FOR PARTICLE AND NUCLEAR PHYSICS Owned and operated as a joint venture by a consortium of Canadian universities via a contribution through the National Research Council Canada LABORATOIRE NATIONAL CANADIEN POUR LA RECHERCHE EN PHYSIQUE NUCLÉAIRE ET EN PHYSIQUE DES PARTICULES Propriété d’un consortium d’universités canadiennes, géré en co-entreprise à partir d’une contribution administrée par le Conseil national de recherches Canada N O 18 F

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CANADA’S NATIONAL LABORATORY FOR PARTICLE AND NUCLEAR PHYSICS. Owned and operated as a joint venture by a consortium of Canadian universities via a contribution through the National Research Council Canada. - PowerPoint PPT Presentation

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Page 1: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

James Inkster, Msc., SFU/TRIUMF

Simplifying the Preparation of 18F-based Biomolecular Imaging Agents Through ‘Click’

Chemistry

CANADA’S NATIONAL LABORATORY FOR PARTICLE AND NUCLEAR PHYSICSOwned and operated as a joint venture by a consortium of Canadian universities via a contribution through the National Research Council Canada

LABORATOIRE NATIONAL CANADIEN POUR LA RECHERCHE EN PHYSIQUE NUCLÉAIRE ET EN PHYSIQUE DES PARTICULES  

Propriété d’un consortium d’universités canadiennes, géré en co-entreprise à partir d’une contribution administrée par le Conseil national de recherches Canada

N

O

18F

Page 2: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

Biomolecules as molecular imaging agents

Why biomolecules? Established synthetic procedures Exquisite specificity

Page 3: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

Biomolecules as molecular imaging agents

Why biomolecules? Established synthetic procedures Exquisite specificity

Why not? Often requires a complex radiosynthesis Certain species may have issues with in

vivo stability, bioavailability Most biomolecules are incompatible with

many radiolabelling protocols

Page 4: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

Direct labelling

"Pre"- labelling

"Post"- labelling

radionuclide

smallmolecule(prostheticgroup)

biomolecule(targeting

agent)

Page 5: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

‘Click’ is a concept

Kolb, H.C. & Sharpless, K.B. Drug Discovery Today 2003, 8, 1128-1137.

1,2,3- triazoles

epoxide ring openings

oximes

hydrazones

N

HN

NH

OH

NO

NN

N

Page 6: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

[18F]FPy5yne: an optimized 18F- based bifunctional molecule

Efficient incorporation of [18F]fluoride via 2-substitued pyridinyl nucleophilic heteroaromatic substitution

Efficient bioconjugation via Huisgen [3+2] cycloaddition reaction

N

O

18FN

O

N -OTf DMSO110 oC, 15 min

K[18F]F-K222

[18F]FPy5yne

Inkster, J. A. H. et al. Journal of Labelled Compounds and Radiopharmaceuticals 2008, 51, 444-452.

Page 7: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

A typical radioTLC

Radiochemical Yield:89.6%±2.0% (n=4)

18F-

N

O

18F

Page 8: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

Peptide labelling with [18F]FPy5yne

N3

O

HN

O

OH

NH

NH2

O

HN

O

NH

NH

HNNH2

O

OH

BG142

[18/19F]FPy5yneCu(ACN)4PF6TBTA

N

O

HN

O

OH

NH

NH2

O

HN

O

NH

NH

HNNH2

O

OH

NN

NF

18/19F-BG142

O

2:1 PBS (pH 7.2): DMF

Page 9: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

Co-injections: (A) [18F]FPy5yne

(B) 18F-Peptide

RCY = 89.6%±2.0% (n =4)(A) (B)

Page 10: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

Proposed biological applications i.e. Where are we going with all this?

18F-BBN [18F-bombesin(7-14)] GRP receptors expressed in ~65% breast

cancers* 18F analogs of bombesin have been prepared

18F-BVD15 NPY1 receptors expressed in 58%-85% breast

cancers* Attractive target, not yet labelled with 18F

18F-Senktide (a NK-3 receptor agonist) Neuropeptide analog of substance P

*Reubi J.C. European Journal of Nuclear Medicine 2002, 29, 855.

Page 11: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

Same Prosthetic Group, Different Biomolecule

P

O

OHO

OHN DNA 20mer

O

N3

P

O

OHO

OHN DNA 20mer

O

N

NNO

N F

[18/19F]FPy5yneCuBrTBTA

2,6-lutidine

4:1 PBS:DMF

N3-ODN1

18/19F-ODN1

Page 12: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

Why make radioactive DNA?

Robinson, R. PLoS Biology, 2004, 2, 18-20.

Page 13: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

“I’ve seen the future, brother: it is

murder.” –L.Cohen

The challenge: the in vivo delivery of nucleic-acid based radiotracers into target cells, followed by retention of the probe by an antisense mechanism

Abes, R. et al., Journal of Peptide Science 2008, 14, 455-460.

Juliano, R. et al. Nucleic Acids Research 2008, 36, 4158-4171.

Debart, F. et al. Current Topics in Medicinal Chemistry 2007, 7, 727-737.

Page 14: Simplifying the Preparation of  18 F-based Biomolecular Imaging Agents Through ‘Click’ Chemistry

Conclusion & Acknowledgements

The goal: to employ TRIUMF LS’s expertise in synthetic organic and radiochemistry to develop simple, efficient and high-impact protocols for the preparation of biological radiopharmaceuticals

The Team PET Group (TRIUMF) Tim Storr (SFU) Mike Adam

(UBC/TRIUMF) David Perrin (UBC) François Bernard (BC

Cancer) Brigitte Guérin (U. de

Sherbrooke) Tom Ruth