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Enzyme mediated incorporation of zirconium-89 or copper-64 into a fragment antibody for same day imaging of epidermal growth factor receptor
Authors:Stacey E. Rudd  Jessica K. Van Zuylekom  Anna Raicevic  Lesley A. Pearce  Carleen Cullinane  Charlotte C. Williams  Timothy E. Adams  Rodney J. Hicks  Paul S. Donnelly
Affiliation:School of Chemistry and Bio21 Molecular Science, Biotechnology Institute University of Melbourne, Parkville Victoria 3010 Australia.; Research Division, Peter MacCallum Cancer Centre, Melbourne Victoria 3000 Australia ; CSIRO Manufacturing, Parkville Victoria 3052 Australia ; Sir Peter MacCallum Department of Oncology, University of Melbourne, Parkville Victoria Australia
Abstract:
Identification of tumors which over-express Epidermal Growth Factor Receptor (EGFR) is important in selecting patients for anti-EGFR therapies. Enzymatic bioconjugation was used to introduce positron-emitting radionuclides (89Zr, 64Cu) into an anti-EGFR antibody fragment for Positron Emission Tomography (PET) imaging the same day as injection. A monovalent antibody fragment with high affinity for EGFR was engineered to include a sequence that is recognized by the transpeptidase sortase A. Two different metal chelators, one for 89ZrIV and one for 64CuII, were modified with a N-terminal glycine to enable them to act as substrates in sortase A mediated bioconjugation to the antibody fragment. Both fragments provided high-quality PET images of EGFR positive tumors in a mouse model at 3 hours post-injection, a significant advantage when compared to radiolabeled full antibodies that require several days between injection of the tracer and imaging. The use of enzymatic bioconjugation gives reproducible homogeneous products with the metal complexes selectively installed on the C-terminus of the antibody potentially simplifying regulatory approval.

Enzymatic bioconjugation to introduce positron-emitting radionuclides (89Zr, 64Cu) into an anti-EGFR antibody fragment allows same day imaging with positron emission tomography.
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