Literature DB >> 17503854

Dual magnetic-/temperature-responsive nanoparticles for microfluidic separations and assays.

James J Lai1, John M Hoffman, Mitsuhiro Ebara, Allan S Hoffman, Claude Estournès, Alain Wattiaux, Patrick S Stayton.   

Abstract

A stimuli-responsive magnetic nanoparticle system for diagnostic target capture and concentration has been developed for microfluidic lab card settings. Telechelic poly(N-isopropylacrylamide) (PNIPAAm) polymer chains were synthesized with dodecyl tails at one end and a reactive carboxylate at the opposite end by the reversible addition fragmentation transfer technique. These PNIPAAm chains self-associate into nanoscale micelles that were used as dimensional confinements to synthesize the magnetic nanoparticles. The resulting superparamagnetic nanoparticles exhibit a gamma-Fe2O3 core ( approximately 5 nm) with a layer of carboxylate-terminated PNIPAAm chains as a corona on the surface. The carboxylate group was used to functionalize the magnetic nanoparticles with biotin and subsequently with streptavidin. The functionalized magnetic nanoparticles can be reversibly aggregated in solution as the temperature is cycled through the PNIPAAm lower critical solution temperature (LCST). While the magnetophoretic mobility of the individual nanoparticles below the LCST is negligible, the aggregates formed above the LCST are large enough to respond to an applied magnetic field. The magnetic nanoparticles can associate with biotinylated targets as individual particles, and then subsequent application of a combined temperature increase and magnetic field can be used to magnetically separate the aggregated particles onto the poly(ethylene glycol)-modified polydimethylsiloxane channel walls of a microfluidic device. When the magnetic field is turned off and the temperature is reversed, the captured aggregates redisperse into the channel flow stream for further downstream processing. The dual magnetic- and temperature-responsive nanoparticles can thus be used as soluble reagents to capture diagnostic targets at a controlled time point and channel position. They can then be isolated and released after the nanoparticles have captured target molecules, overcoming the problem of low magnetophoretic mobility of the individual particle while retaining the advantages of a high surface to volume ratio and faster diffusive properties during target capture.

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Year:  2007        PMID: 17503854     DOI: 10.1021/la062527g

Source DB:  PubMed          Journal:  Langmuir        ISSN: 0743-7463            Impact factor:   3.882


  25 in total

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2.  Mixed stimuli-responsive magnetic and gold nanoparticle system for rapid purification, enrichment, and detection of biomarkers.

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4.  Multiplexed enrichment and detection of malarial biomarkers using a stimuli-responsive iron oxide and gold nanoparticle reagent system.

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5.  Human Immunodeficiency Virus (HIV) Separation and Enrichment via the Combination of Antiviral Lectin Recognition and a Thermoresponsive Reagent System.

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6.  Surface design with self-heating smart polymers for on-off switchable traps.

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7.  Temperature-responsive electrospun nanofibers for 'on-off' switchable release of dextran.

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8.  "Smart" diblock copolymers as templates for magnetic-core gold-shell nanoparticle synthesis.

Authors:  Michael A Nash; James J Lai; Allan S Hoffman; Paul Yager; Patrick S Stayton
Journal:  Nano Lett       Date:  2010-01       Impact factor: 11.189

9.  Hybrid biofunctional nanostructures as stimuli-responsive catalytic systems.

Authors:  Gernot U Marten; Thorsten Gelbrich; Annette M Schmidt
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10.  Synthesis, characterization, and in vitro evaluation of novel polymer-coated magnetic nanoparticles for controlled delivery of doxorubicin.

Authors:  Abolfazl Akbarzadeh; Nosratollah Zarghami; Haleh Mikaeili; Davoud Asgari; Amir Mohammad Goganian; Hanie Khaksar Khiabani; Mohammad Samiei; Soodabeh Davaran
Journal:  Nanotechnol Sci Appl       Date:  2012-02-07
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