3D-printed microfluidics integrated with optical nanostructured porous aptasensors for protein detection

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dc.identifier.uri http://dx.doi.org/10.15488/12294
dc.identifier.uri https://www.repo.uni-hannover.de/handle/123456789/12392
dc.contributor.author Arshavsky-Graham, Sofia
dc.contributor.author Enders, Anton
dc.contributor.author Ackerman, Shanny
dc.contributor.author Bahnemann, Janina
dc.contributor.author Segal, Ester
dc.date.accessioned 2022-06-21T05:47:16Z
dc.date.available 2022-06-21T05:47:16Z
dc.date.issued 2021
dc.identifier.citation Arshavsky-Graham, S.; Enders, A.; Ackerman, S.; Bahnemann, J.; Segal, E.: 3D-printed microfluidics integrated with optical nanostructured porous aptasensors for protein detection. In: Microchimica Acta 188 (2021), Nr. 3, 67. DOI: https://doi.org/10.1007/s00604-021-04725-0
dc.description.abstract Microfluidic integration of biosensors enables improved biosensing performance and sophisticated lab-on-a-chip platform design for numerous applications. While soft lithography and polydimethylsiloxane (PDMS)-based microfluidics are still considered the gold standard, 3D-printing has emerged as a promising fabrication alternative for microfluidic systems. Herein, a 3D-printed polyacrylate-based microfluidic platform is integrated for the first time with a label-free porous silicon (PSi)–based optical aptasensor via a facile bonding method. The latter utilizes a UV-curable adhesive as an intermediate layer, while preserving the delicate nanostructure of the porous regions within the microchannels. As a proof-of-concept, a generic model aptasensor for label-free detection of his-tagged proteins is constructed, characterized, and compared to non-microfluidic and PDMS-based microfluidic setups. Detection of the target protein is carried out by real-time monitoring reflectivity changes of the PSi, induced by the target binding to the immobilized aptamers within the porous nanostructure. The microfluidic integrated aptasensor has been successfully used for detection of a model target protein, in the range 0.25 to 18 μM, with a good selectivity and an improved limit of detection, when compared to a non-microfluidic biosensing platform (0.04 μM vs. 2.7 μM, respectively). Furthermore, a superior performance of the 3D-printed microfluidic aptasensor is obtained, compared to a conventional PDMS-based microfluidic platform with similar dimensions. Graphical abstract: [Figure not available: see fulltext.]. © 2021, The Author(s). eng
dc.language.iso eng
dc.publisher Wien [u.a.] : Springer
dc.relation.ispartofseries Microchimica Acta 188 (2021), Nr. 3
dc.rights CC BY 4.0 Unported
dc.rights.uri https://creativecommons.org/licenses/by/4.0/
dc.subject 3D-printing eng
dc.subject Biosensor eng
dc.subject Microfluidics eng
dc.subject PDMS eng
dc.subject Polyacrylate eng
dc.subject Porous silicon eng
dc.subject acrylic acid resin eng
dc.subject aptamer eng
dc.subject carbopol 940 eng
dc.subject glycosidase eng
dc.subject immobilized nucleic acid eng
dc.subject silicon eng
dc.subject chemistry eng
dc.subject devices eng
dc.subject genetic procedures eng
dc.subject lab on a chip eng
dc.subject limit of detection eng
dc.subject microfluidic analysis eng
dc.subject porosity eng
dc.subject procedures eng
dc.subject proof of concept eng
dc.subject three dimensional printing eng
dc.subject Acrylic Resins eng
dc.subject Aptamers, Nucleotide eng
dc.subject Biosensing Techniques eng
dc.subject Glycoside Hydrolases eng
dc.subject Immobilized Nucleic Acids eng
dc.subject Lab-On-A-Chip Devices eng
dc.subject Limit of Detection eng
dc.subject Microfluidic Analytical Techniques eng
dc.subject Porosity eng
dc.subject Printing, Three-Dimensional eng
dc.subject Proof of Concept Study eng
dc.subject Silicon eng
dc.subject.ddc 540 | Chemie ger
dc.title 3D-printed microfluidics integrated with optical nanostructured porous aptasensors for protein detection
dc.type Article
dc.type Text
dc.relation.essn 1436-5073
dc.relation.doi https://doi.org/10.1007/s00604-021-04725-0
dc.bibliographicCitation.issue 3
dc.bibliographicCitation.volume 188
dc.bibliographicCitation.firstPage 67
dc.description.version publishedVersion
tib.accessRights frei zug�nglich


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