Drug screening of cancer cell lines and human primary tumors using droplet microfluidics

Drug screening of cancer cell lines and human primary tumors using droplet microfluidics

Abstract Precision Medicine in Oncology requires tailoring of therapeutic strategies to individual cancer patients. Due to the limited quantity of tumor samples, this proves to be difficult, especially for early stage cancer patients whose tumors are small. In this study, we exploited a 2.4 × 2.4 ce...

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Main Authors: Ada Hang-Heng Wong, Haoran Li, Yanwei Jia, Pui-In Mak, Rui Paulo da Silva Martins, Yan Liu, Chi Man Vong, Hang Cheong Wong, Pak Kin Wong, Haitao Wang, Heng Sun, Chu-Xia Deng
Format: Article
Language:English
Published: Nature Publishing Group 2017-08-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-017-08831-z
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spelling doaj-09904b3aa3004ace89370e211250ec322020-12-08T01:04:22ZengNature Publishing GroupScientific Reports2045-23222017-08-017111510.1038/s41598-017-08831-zDrug screening of cancer cell lines and human primary tumors using droplet microfluidicsAda Hang-Heng Wong0Haoran Li1Yanwei Jia2Pui-In Mak3Rui Paulo da Silva Martins4Yan Liu5Chi Man Vong6Hang Cheong Wong7Pak Kin Wong8Haitao Wang9Heng Sun10Chu-Xia Deng11Cancer Centre, Faculty of Health Sciences, University of MacauState-Key Laboratory of Analog and Mixed-Signal VLSI (AMSV), University of MacauState-Key Laboratory of Analog and Mixed-Signal VLSI (AMSV), University of MacauState-Key Laboratory of Analog and Mixed-Signal VLSI (AMSV), University of MacauState-Key Laboratory of Analog and Mixed-Signal VLSI (AMSV), University of MacauDepartment of Computer and Information Science, Faculty of Science and Technology, University of MacauDepartment of Computer and Information Science, Faculty of Science and Technology, University of MacauDepartment of Electromechanical Engineering, Faculty of Science and Technology, University of MacauDepartment of Electromechanical Engineering, Faculty of Science and Technology, University of MacauCancer Centre, Faculty of Health Sciences, University of MacauCancer Centre, Faculty of Health Sciences, University of MacauCancer Centre, Faculty of Health Sciences, University of MacauAbstract Precision Medicine in Oncology requires tailoring of therapeutic strategies to individual cancer patients. Due to the limited quantity of tumor samples, this proves to be difficult, especially for early stage cancer patients whose tumors are small. In this study, we exploited a 2.4 × 2.4 centimeters polydimethylsiloxane (PDMS) based microfluidic chip which employed droplet microfluidics to conduct drug screens against suspended and adherent cancer cell lines, as well as cells dissociated from primary tumor of human patients. Single cells were dispersed in aqueous droplets and imaged within 24 hours of drug treatment to assess cell viability by ethidium homodimer 1 staining. Our results showed that 5 conditions could be screened for every 80,000 cells in one channel on our chip under current circumstances. Additionally, screening conditions have been adapted to both suspended and adherent cancer cells, giving versatility to potentially all types of cancers. Hence, this study provides a powerful tool for rapid, low-input drug screening of primary cancers within 24 hours after tumor resection from cancer patients. This paves the way for further technological advancement to cutting down sample size and increasing drug screening throughput in advent to personalized cancer therapy.https://doi.org/10.1038/s41598-017-08831-z
collection DOAJ
language English
format Article
sources DOAJ
author Ada Hang-Heng Wong
Haoran Li
Yanwei Jia
Pui-In Mak
Rui Paulo da Silva Martins
Yan Liu
Chi Man Vong
Hang Cheong Wong
Pak Kin Wong
Haitao Wang
Heng Sun
Chu-Xia Deng
spellingShingle Ada Hang-Heng Wong
Haoran Li
Yanwei Jia
Pui-In Mak
Rui Paulo da Silva Martins
Yan Liu
Chi Man Vong
Hang Cheong Wong
Pak Kin Wong
Haitao Wang
Heng Sun
Chu-Xia Deng
Drug screening of cancer cell lines and human primary tumors using droplet microfluidics
Scientific Reports
author_facet Ada Hang-Heng Wong
Haoran Li
Yanwei Jia
Pui-In Mak
Rui Paulo da Silva Martins
Yan Liu
Chi Man Vong
Hang Cheong Wong
Pak Kin Wong
Haitao Wang
Heng Sun
Chu-Xia Deng
author_sort Ada Hang-Heng Wong
title Drug screening of cancer cell lines and human primary tumors using droplet microfluidics
title_short Drug screening of cancer cell lines and human primary tumors using droplet microfluidics
title_full Drug screening of cancer cell lines and human primary tumors using droplet microfluidics
title_fullStr Drug screening of cancer cell lines and human primary tumors using droplet microfluidics
title_full_unstemmed Drug screening of cancer cell lines and human primary tumors using droplet microfluidics
title_sort drug screening of cancer cell lines and human primary tumors using droplet microfluidics
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2017-08-01
description Abstract Precision Medicine in Oncology requires tailoring of therapeutic strategies to individual cancer patients. Due to the limited quantity of tumor samples, this proves to be difficult, especially for early stage cancer patients whose tumors are small. In this study, we exploited a 2.4 × 2.4 centimeters polydimethylsiloxane (PDMS) based microfluidic chip which employed droplet microfluidics to conduct drug screens against suspended and adherent cancer cell lines, as well as cells dissociated from primary tumor of human patients. Single cells were dispersed in aqueous droplets and imaged within 24 hours of drug treatment to assess cell viability by ethidium homodimer 1 staining. Our results showed that 5 conditions could be screened for every 80,000 cells in one channel on our chip under current circumstances. Additionally, screening conditions have been adapted to both suspended and adherent cancer cells, giving versatility to potentially all types of cancers. Hence, this study provides a powerful tool for rapid, low-input drug screening of primary cancers within 24 hours after tumor resection from cancer patients. This paves the way for further technological advancement to cutting down sample size and increasing drug screening throughput in advent to personalized cancer therapy.
url https://doi.org/10.1038/s41598-017-08831-z
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