Fabrication routes via projection stereolithography for 3D-printing of microfluidic geometries for nucleic acid amplification.

Fabrication routes via projection stereolithography for 3D-printing of microfluidic geometries for nucleic acid amplification.

Digital Light Processing (DLP) stereolithography (SLA) as a high-resolution 3D printing process offers a low-cost alternative for prototyping of microfluidic geometries, compared to traditional clean-room and workshop-based methods. Here, we investigate DLP-SLA printing performance for the productio...

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Main Authors: Charalampos Tzivelekis, Pavlos Sgardelis, Kevin Waldron, Richard Whalley, Dehong Huo, Kenny Dalgarno
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2020-01-01
Series:PLoS ONE
Online Access:https://doi.org/10.1371/journal.pone.0240237
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spelling doaj-cb9e93b52c1f493bbb15783c494907d22021-03-04T11:08:52ZengPublic Library of Science (PLoS)PLoS ONE1932-62032020-01-011510e024023710.1371/journal.pone.0240237Fabrication routes via projection stereolithography for 3D-printing of microfluidic geometries for nucleic acid amplification.Charalampos TzivelekisPavlos SgardelisKevin WaldronRichard WhalleyDehong HuoKenny DalgarnoDigital Light Processing (DLP) stereolithography (SLA) as a high-resolution 3D printing process offers a low-cost alternative for prototyping of microfluidic geometries, compared to traditional clean-room and workshop-based methods. Here, we investigate DLP-SLA printing performance for the production of micro-chamber chip geometries suitable for Polymerase Chain Reaction (PCR), a key process in molecular diagnostics to amplify nucleic acid sequences. A DLP-SLA fabrication protocol for printed micro-chamber devices with monolithic micro-channels is developed and evaluated. Printed devices were post-processed with ultraviolet (UV) light and solvent baths to reduce PCR inhibiting residuals and further treated with silane coupling agents to passivate the surface, thereby limiting biomolecular adsorption occurences during the reaction. The printed devices were evaluated on a purpose-built infrared (IR) mediated PCR thermocycler. Amplification of 75 base pair long target sequences from genomic DNA templates on fluorosilane and glass modified chips produced amplicons consistent with the control reactions, unlike the non-silanized chips that produced faint or no amplicon. The results indicated good functionality of the IR thermocycler and good PCR compatibility of the printed and silanized SLA polymer. Based on the proposed methods, various microfluidic designs and ideas can be validated in-house at negligible costs without the requirement of tool manufacturing and workshop or clean-room access. Additionally, the versatile chemistry of 3D printing resins enables customised surface properties adding significant value to the printed prototypes. Considering the low setup and unit cost, design flexibility and flexible resin chemistries, DLP-SLA is anticipated to play a key role in future prototyping of microfluidics, particularly in the fields of research biology and molecular diagnostics. From a system point-of-view, the proposed method of thermocycling shows promise for portability and modular integration of funcitonalitites for diagnostic or research applications that utilize nucleic acid amplification technology.https://doi.org/10.1371/journal.pone.0240237
collection DOAJ
language English
format Article
sources DOAJ
author Charalampos Tzivelekis
Pavlos Sgardelis
Kevin Waldron
Richard Whalley
Dehong Huo
Kenny Dalgarno
spellingShingle Charalampos Tzivelekis
Pavlos Sgardelis
Kevin Waldron
Richard Whalley
Dehong Huo
Kenny Dalgarno
Fabrication routes via projection stereolithography for 3D-printing of microfluidic geometries for nucleic acid amplification.
PLoS ONE
author_facet Charalampos Tzivelekis
Pavlos Sgardelis
Kevin Waldron
Richard Whalley
Dehong Huo
Kenny Dalgarno
author_sort Charalampos Tzivelekis
title Fabrication routes via projection stereolithography for 3D-printing of microfluidic geometries for nucleic acid amplification.
title_short Fabrication routes via projection stereolithography for 3D-printing of microfluidic geometries for nucleic acid amplification.
title_full Fabrication routes via projection stereolithography for 3D-printing of microfluidic geometries for nucleic acid amplification.
title_fullStr Fabrication routes via projection stereolithography for 3D-printing of microfluidic geometries for nucleic acid amplification.
title_full_unstemmed Fabrication routes via projection stereolithography for 3D-printing of microfluidic geometries for nucleic acid amplification.
title_sort fabrication routes via projection stereolithography for 3d-printing of microfluidic geometries for nucleic acid amplification.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2020-01-01
description Digital Light Processing (DLP) stereolithography (SLA) as a high-resolution 3D printing process offers a low-cost alternative for prototyping of microfluidic geometries, compared to traditional clean-room and workshop-based methods. Here, we investigate DLP-SLA printing performance for the production of micro-chamber chip geometries suitable for Polymerase Chain Reaction (PCR), a key process in molecular diagnostics to amplify nucleic acid sequences. A DLP-SLA fabrication protocol for printed micro-chamber devices with monolithic micro-channels is developed and evaluated. Printed devices were post-processed with ultraviolet (UV) light and solvent baths to reduce PCR inhibiting residuals and further treated with silane coupling agents to passivate the surface, thereby limiting biomolecular adsorption occurences during the reaction. The printed devices were evaluated on a purpose-built infrared (IR) mediated PCR thermocycler. Amplification of 75 base pair long target sequences from genomic DNA templates on fluorosilane and glass modified chips produced amplicons consistent with the control reactions, unlike the non-silanized chips that produced faint or no amplicon. The results indicated good functionality of the IR thermocycler and good PCR compatibility of the printed and silanized SLA polymer. Based on the proposed methods, various microfluidic designs and ideas can be validated in-house at negligible costs without the requirement of tool manufacturing and workshop or clean-room access. Additionally, the versatile chemistry of 3D printing resins enables customised surface properties adding significant value to the printed prototypes. Considering the low setup and unit cost, design flexibility and flexible resin chemistries, DLP-SLA is anticipated to play a key role in future prototyping of microfluidics, particularly in the fields of research biology and molecular diagnostics. From a system point-of-view, the proposed method of thermocycling shows promise for portability and modular integration of funcitonalitites for diagnostic or research applications that utilize nucleic acid amplification technology.
url https://doi.org/10.1371/journal.pone.0240237
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