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Journal ArticleDOI

Solution-phase surface modification in intact poly(dimethylsiloxane) microfluidic channels.

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TLDR
An improved approach composed of an oxidation reaction in acidic H2O2 solution and a sequential silanization reaction using neat silane reagents for surface modification of poly(dimethylsiloxane) (PDMS) substrates was developed, indicating that the PEG-grafted PDMS surfaces exhibit improved short-term surface dynamics and robust long-term stability.
Abstract
An improved approach composed of an oxidation reaction in acidic H2O2 solution and a sequential silanization reaction using neat silane reagents for surface modification of poly(dimethylsiloxane) (PDMS) substrates was developed. This solution-phase approach is simple and convenient for some routine analytical applications in chemistry and biology laboratories and is designed for intact PDMS-based microfluidic devices, with no device postassembly required. Using this improved approach, two different functional groups, poly(ethylene glycol) (PEG) and amine (NH2), were introduced onto PDMS surfaces for passivation of nonspecific protein absorption and attachment of biomolecules, respectively. X-ray electron spectroscopy and temporal contact angle experiments were employed to monitor functional group transformation and dynamic characteristics of the PEG-grafted PDMS substrates; fluorescent protein solutions were introduced into the PEG-grafted PDMS microchannels to test their protein repelling characteristics. These analytical data indicate that the PEG-grafted PDMS surfaces exhibit improved short-term surface dynamics and robust long-term stability. The amino-grafted PDMS microchannels are also relatively stable and can be further activated for modifications with peptide, DNA, and protein on the surfaces of microfluidic channels. The resulting biomolecule-grafted PDMS microchannels can be utilized for cell immobilization and incubation, semiquantitative DNA hybridization, and immunoassay.

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Journal ArticleDOI

Recent developments in PDMS surface modification for microfluidic devices

TL;DR: This review will present recent research on surface modifications of PDMS using techniques ranging from metal layer coatings and layer‐by‐layer depositions to dynamic surfactant treatments and the adsorption of amphipathic proteins.
Journal ArticleDOI

Advances in microfluidic materials, functions, integration, and applications.

TL;DR: The successful demonstration of electrophoresis and electroosmotic pumping in a microfluidic device provided a nonmechanical method for both fluid control and separation, and integration of multiple processes can be highly enabling for many applications.
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Surface molecular property modifications for poly(dimethylsiloxane) (PDMS) based microfluidic devices

TL;DR: Recent advances in nonbiofouling PDMS surface modification strategies applicable to microfluidic technology are summarized and two main categories are classified: physical approach including physisorption of charged or amphiphilic polymers and copolymers, as well as chemical approach including self assembled monolayer and thick polymer coating.
Journal ArticleDOI

Protein immobilization techniques for microfluidic assays

TL;DR: A review of immobilization methods and chemistries, and discusses studies exemplar of key approaches, considers the microfluidics literature from 1997 to present, and describes multifunctional surface coatings that can perform tasks that were, until recently, relegated to multiple functional coatings.
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Current development in microfluidic immunosensing chip.

TL;DR: The emerging microfludic immunosensor technology may be a promising prospect that can propel the improvement of clinical and medical diagnosis.
References
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Monolithic microfabricated valves and pumps by multilayer soft lithography

TL;DR: An extension to the soft lithography paradigm, multilayersoft lithography, with which devices consisting of multiple layers may be fabricated from soft materials is described, to build active microfluidic systems containing on-off valves, switching valves, and pumps entirely out of elastomer.
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Cell attachment activity of fibronectin can be duplicated by small synthetic fragments of the molecule

TL;DR: The ability of fibronectin to bind cells can be accounted for by the tetrapeptide L-arginyl-glycyl- L-aspartyl-L-serine, a sequence which is part of the cell attachment domain of fibronsectin and present in at least five other proteins.
Journal ArticleDOI

Prostate stem cell antigen: A cell surface marker overexpressed in prostate cancer

TL;DR: Flow cytometric analysis demonstrates that PSCA is expressed predominantly on the cell surface and is anchored by a GPI linkage, which supports P SCA as a target for prostate cancer diagnosis and therapy.
Journal ArticleDOI

Direct measurement of interfacial interactions between semispherical lenses and flat sheets of poly(dimethylsiloxane) and their chemical derivatives

TL;DR: In this article, a theory of Johnson, Kendall and Roberts was used to obtain the works of adhesion between PDMS suifaces in the air and liquid media, which was consistent with the value obtained from measurements made in air and with the analysis of the contact angles of nonpolar liquids on PDMS using the Good-Girifalco-Fowkes equation.
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