Issue 18, 2015

Upconverting nanoparticle to quantum dot FRET for homogeneous double-nano biosensors

Abstract

Both upconverting nanoparticles (UCNPs) and semiconductor quantum dots (QDs) have revolutionized optical biosensing because of their unique photophysical properties. However, their outstanding photostability, near-infrared (NIR) excitability, and colour tunability have never been combined for homogeneous mix-and-measure FRET (Förster resonance energy transfer) biosensors that do not require any washing or separation steps. Here we demonstrate that UCNP-to-QD FRET systems can be used for rapid homogeneous bioassays, which are essential tools for clinical diagnostics. One of the main drawbacks of UCNPs for FRET, namely their very low photoluminescence (PL) quantum yields, was efficiently overcome by using QD FRET acceptors with very strong spectral overlap with the UCNP donors. This resulted in unrivalled Förster distances for UCNP-based FRET pairs of up to 6 nm. We could quantify the prototypical analyte biotin (vitamin H) at low nanomolar concentrations and steady-state and time-resolved PL analysis showed that UCNP-to-QD FRET was caused by streptavidin-to-biotin binding. Immediate applicability in biosensing was demonstrated by biotin replacement assays over a large concentration range with IC50 values between 8 nM and 250 nM and detection limits down to 5 nM. The high photostability of the double-nanoparticle biosensor, the NIR excitation of UCNPs for minimal autofluorescence, and the spectral multiplexing capability of QDs offer a large potential for spectroscopy and imaging-based biosensing beyond in vitro diagnostics.

Graphical abstract: Upconverting nanoparticle to quantum dot FRET for homogeneous double-nano biosensors

Supplementary files

Article information

Article type
Paper
Submitted
18 Nov 2014
Accepted
16 Jan 2015
First published
16 Jan 2015

RSC Adv., 2015,5, 13270-13277

Upconverting nanoparticle to quantum dot FRET for homogeneous double-nano biosensors

L. Mattsson, K. D. Wegner, N. Hildebrandt and T. Soukka, RSC Adv., 2015, 5, 13270 DOI: 10.1039/C5RA00397K

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