Iodide-doped precious metal nanoparticles: measuring oxidative stress in vivo via photoacoustic imaging

Accumulation of reactive oxygen and nitrogen species (RONS) can induce cell damage and even cell death. RONS are short-lived species, which makes direct, precise, and real-time measurement difficult. Biologically-relevant RONS levels are in the nM-μM scale; hence, there is a need for highly sensitiv...

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Bibliographic Details
Published in:Nanoscale 2020-05, Vol.12 (19), p.10511-10520
Main Authors: Mantri, Yash, Davidi, Barak, Lemaster, Jeanne E, Hariri, Ali, Jokerst, Jesse V
Format: Article
Language:English
Subjects:
Animals
Biocompatibility
Cell death
Doping
Electrochemical analysis
Fluorescence
Gold
Hydrogen Peroxide
Imaging
Iodides
Metal Nanoparticles - toxicity
Mice
Nanoparticles
Nanorods
Oxidation
Oxidative Stress
Photoacoustic Techniques
Sensitivity
Silver
Toxicity
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Summary:Accumulation of reactive oxygen and nitrogen species (RONS) can induce cell damage and even cell death. RONS are short-lived species, which makes direct, precise, and real-time measurement difficult. Biologically-relevant RONS levels are in the nM-μM scale; hence, there is a need for highly sensitive RONS probes. We previously used hybrid gold-core silver-shell nanoparticles with mM sensitivity to H2O2. These particles reported the presence of RONS via spectral shifts which could easily be quantified via photoacoustic imaging. Here, we used halide doping to tune the electrochemical properties of these materials to better match the oxidation potential of RONS. This work describes the synthesis, characterization, and application of these AgI-coated gold nanorods (AgI/AuNR). The I : Ag molar ratio, pH, and initial Ag shell thickness were optimized for good RONS detection limits. Halide doping lowers the reduction potential of Ag from to resulting in a 1000-fold increase in H2O2 and 100 000-fold increase in ONOO- sensitivity. The AgI/AuNR system also etches 45-times faster than undoped Ag/AuNR. The AgI/AuNR easily reported the endogenously produced RONS in established cells lines as well as murine models.
ISSN:2040-3364
2040-3372
DOI:10.1039/d0nr03047c