Critical design issues in the targeted molecular imaging of cell surface receptors

Sim, N.; Parker, D.

doi:10.1039/c4cs00364k

Critical design issues in the targeted molecular imaging of cell surface receptors

Sim, N.; Parker, D.

Authors

N. Sim

David Parker david.parker@durham.ac.uk
Emeritus Professor

Abstract

The imaging of cell-surface receptors can be achieved using several methods, including single photon emission tomography (SPECT) positron emission tomography (PET), optical imaging and magnetic resonance imaging (MRI). The application of targeted MRI contrast agents is particularly well-suited to this task, provided that the agents reach the desired site efficiently and selectively. In addition, they should bind reversibly to the cell-surface receptor and give rise to a large change in cellular relaxation rate, in competition with binding to the natural substrate. Such approaches offer promise in the molecular imaging of neurotransmission in the brain, using conjugates that selectively target dopamine or glutamate receptor sub-types. Strategies based on the use of competitive antagonist vectors offer particular scope, as such conjugates are generally not taken into the target cell following cell surface receptor binding, in contrast to the use of MRI contrast agents based on agonists that tend to be internalised quickly or are designed to target intracellular sites.

Citation

Sim, N., & Parker, D. (2015). Critical design issues in the targeted molecular imaging of cell surface receptors. Chemical Society Reviews, 44(8), 2122-2134. https://doi.org/10.1039/c4cs00364k

Journal Article Type	Article
Publication Date	Apr 21, 2015
Deposit Date	Feb 27, 2015
Publicly Available Date	Aug 19, 2015
Journal	Chemical Society Reviews
Print ISSN	0306-0012
Electronic ISSN	1460-4744
Publisher	Royal Society of Chemistry
Peer Reviewed	Peer Reviewed
Volume	44
Issue	8
Pages	2122-2134
DOI	https://doi.org/10.1039/c4cs00364k
Public URL	https://durham-repository.worktribe.com/output/1412070