Reported
by: Aviral Vatsa
Authors:
Nicole M. Iverson, Paul W. Barone, Mia Shandell, Laura J. Trudel, Selda Sen, Fatih Sen, Vsevolod Ivanov, Esha Atolia, Edgardo Farias, Thomas P. McNicholas, Nigel Reuel, Nicola M. A. Parry, Gerald N. Wogan & Michael S. Strano
Nature Nanotechnology doi:10.1038/nnano.2013.222
Abstract
Single-walled
carbon nanotubes are particularly attractive for biomedical
applications, because they exhibit a fluorescent signal in a spectral
region where there is minimal interference from biological media.
Although single-walled carbon nanotubes have been used as highly
sensitive detectors for various compounds, their use as in
vivo biomarkers
requires the simultaneous optimization of various parameters,
including biocompatibility, molecular recognition, high fluorescence
quantum efficiency and signal transduction. Here we show that a
polyethylene glycol ligated copolymer stabilizes
near-infrared-fluorescent single-walled carbon nanotubes sensors in
solution, enabling intravenous injection into mice and the selective
detection of local nitric oxide concentration with a detection limit
of 1 µM. The half-life for liver retention is 4 h, with
sensors clearing the lungs within 2 h after injection, thus
avoiding a dominant route of in
vivo nanotoxicology.
After localization within the liver, it is possible to follow the
transient inflammation using nitric oxide as a marker and signalling
molecule. To this end, we also report a spatial-spectral imaging
algorithm to deconvolute fluorescence intensity and spatial
information from measurements. Finally, we demonstrate that
alginate-encapsulated single-walled carbon nanotubes can function as
implantable inflammation sensors for nitric oxide detection, with no
intrinsic immune reactivity or other adverse response for more than
400 days.
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