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Nanoparticle-mediated measurement of target-drug binding in cancer cells.


ABSTRACT: Responses to molecularly targeted therapies can be highly variable and depend on mutations, fluctuations in target protein levels in individual cells, and drug delivery. The ability to rapidly quantitate drug response in cells harvested from patients in a point-of-care setting would have far reaching implications. Capitalizing on recent developments with miniaturized NMR technologies, we have developed a magnetic nanoparticle-based approach to directly measure both target expression and drug binding in scant human cells. The method involves covalent conjugation of the small-molecule drug to a magnetic nanoparticle that is then used as a read-out for target expression and drug-binding affinity. Using poly(ADP-ribose) polymerase (PARP) inhibition as a model system, we developed an approach to distinguish differential expression of PARP in scant cells with excellent correlation to gold standards, the ability to mimic drug pharmacodynamics ex vivo through competitive target-drug binding, and the potential to perform such measurements in clinical samples.

SUBMITTER: Ullal AV 

PROVIDER: S-EPMC3297118 | biostudies-literature | 2011 Nov

REPOSITORIES: biostudies-literature

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Nanoparticle-mediated measurement of target-drug binding in cancer cells.

Ullal Adeeti V AV   Reiner Thomas T   Yang Katherine S KS   Gorbatov Rostic R   Min Changwook C   Issadore David D   Lee Hakho H   Weissleder Ralph R  

ACS nano 20111013 11


Responses to molecularly targeted therapies can be highly variable and depend on mutations, fluctuations in target protein levels in individual cells, and drug delivery. The ability to rapidly quantitate drug response in cells harvested from patients in a point-of-care setting would have far reaching implications. Capitalizing on recent developments with miniaturized NMR technologies, we have developed a magnetic nanoparticle-based approach to directly measure both target expression and drug bin  ...[more]

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