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research article

Evaluating Cellular Drug Uptake with Fluorescent Sensor Proteins

Scarabelli, Silvia  
•
Tan, Kui Thong  
•
Griss, Rudolf  
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2017
ACS Sensors

We are introducing a new approach to evaluate cellular uptake of drugs and drug candidates into living cells. The approach is based on converting the protein target of a given class of compounds into a fluorescent biosensor. By measuring the binding of different compounds to their cognate biosensor in live cells and comparing these values to those measured in vitro, their cellular uptake and concentrations can be ranked. We demonstrate that our strategy enables the evaluation of the cellular uptake into the cytosol of 2 classes of inhibitors using two different sensor designs; first, sensors comprising the self-labeling protein SNAP conjugated with a chemically modified inhibitor shown for inhibitors of the enzyme human carbonic anhydrase II; and a label-free sensor for inhibitors of protein−protein interactions demonstrated for the protein pair p53−HDM2.

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Type
research article
DOI
10.1021/acssensors.7b00331
Web of Science ID

WOS:000408702500015

Author(s)
Scarabelli, Silvia  
Tan, Kui Thong  
Griss, Rudolf  
Hovius, Ruud  
D’Alessandro, Pier Luca
Vorherr, Thomas
Johnsson, Kai  
Date Issued

2017

Publisher

Amer Chemical Soc

Published in
ACS Sensors
Volume

2

Issue

8

Start page

1191

End page

1197

Subjects

intracellular concentration

•

FRET-based sensor protein

•

cellular absorption

•

cellular clearance

•

HCAII

•

p53-HDM2 interaction

•

peptide therapeutics

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LIP  
Available on Infoscience
August 14, 2017
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/139642
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