Organ-on-a-Chip Platforms for Drug Screening and Delivery in Tumor Cells: A Systematic Review

Inês M. Gonçalves; Violeta Carvalho; Raquel O. Rodrigues; Diana Pinho; Senhorinha F.C.F. Teixeira; Ana Moita; Takeshi Hori; Hirokazu Kaji; Rui Lima; Graça Minas

doi:10.3390/cancers14040935

Organ-on-a-Chip Platforms for Drug Screening and Delivery in Tumor Cells: A Systematic Review

Inês M. Gonçalves, Violeta Carvalho, Raquel O. Rodrigues, Diana Pinho, Senhorinha F.C.F. Teixeira, Ana Moita, Takeshi Hori, Hirokazu Kaji, Rui Lima, Graça Minas

ENG - Finemechanics

Research output: Contribution to journal › Review article › peer-review

14 Citations (Scopus)

Abstract

The development of cancer models that rectify the simplicity of monolayer or static cell cultures physiologic microenvironment and, at the same time, replicate the human system more accurately than animal models has been a challenge in biomedical research. Organ-on-a-chip (OoC) devices are a solution that has been explored over the last decade. The combination of microfluidics and cell culture allows the design of a dynamic microenvironment suitable for the evaluation of treatments’ efficacy and effects, closer to the response observed in patients. This systematic review sums the studies from the last decade, where OoC with cancer cell cultures were used for drug screening assays. The studies were selected from three databases and analyzed following the research guidelines for systematic reviews proposed by PRISMA. In the selected studies, several types of cancer cells were evaluated, and the majority of treatments tested were standard chemotherapeutic drugs. Some studies reported higher drug resistance of the cultures on the OoC devices than on 2D cultures, which indicates the better resemblance to in vivo conditions of the former. Several studies also included the replication of the microvasculature or the combination of different cell cultures. The presence of vasculature can influence positively or negatively the drug efficacy since it con-tributes to a greater diffusion of the drug and also oxygen and nutrients. Co-cultures with liver cells contributed to the evaluation of the systemic toxicity of some drugs metabolites. Nevertheless, few studies used patient cells for the drug screening assays.

Original language	English
Article number	935
Journal	Cancers
Volume	14
Issue number	4
DOIs	https://doi.org/10.3390/cancers14040935
Publication status	Published - 2022 Feb 1

Keywords

Cancer cells
Cell culture
Drug delivery
Drug screening
Hard tissues and organs
Microbioreactor
Microfluidics
Nanoparticles
Organ-on-a-chip
Organoids

ASJC Scopus subject areas

Oncology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3390/cancers14040935

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@article{d8f2d4b7e27c4be5ab2467e3b8f08ef2,

title = "Organ-on-a-Chip Platforms for Drug Screening and Delivery in Tumor Cells: A Systematic Review",

abstract = "The development of cancer models that rectify the simplicity of monolayer or static cell cultures physiologic microenvironment and, at the same time, replicate the human system more accurately than animal models has been a challenge in biomedical research. Organ-on-a-chip (OoC) devices are a solution that has been explored over the last decade. The combination of microfluidics and cell culture allows the design of a dynamic microenvironment suitable for the evaluation of treatments{\textquoteright} efficacy and effects, closer to the response observed in patients. This systematic review sums the studies from the last decade, where OoC with cancer cell cultures were used for drug screening assays. The studies were selected from three databases and analyzed following the research guidelines for systematic reviews proposed by PRISMA. In the selected studies, several types of cancer cells were evaluated, and the majority of treatments tested were standard chemotherapeutic drugs. Some studies reported higher drug resistance of the cultures on the OoC devices than on 2D cultures, which indicates the better resemblance to in vivo conditions of the former. Several studies also included the replication of the microvasculature or the combination of different cell cultures. The presence of vasculature can influence positively or negatively the drug efficacy since it con-tributes to a greater diffusion of the drug and also oxygen and nutrients. Co-cultures with liver cells contributed to the evaluation of the systemic toxicity of some drugs metabolites. Nevertheless, few studies used patient cells for the drug screening assays.",

keywords = "Cancer cells, Cell culture, Drug delivery, Drug screening, Hard tissues and organs, Microbioreactor, Microfluidics, Nanoparticles, Organ-on-a-chip, Organoids",

author = "Gon{\c c}alves, {In{\^e}s M.} and Violeta Carvalho and Rodrigues, {Raquel O.} and Diana Pinho and Teixeira, {Senhorinha F.C.F.} and Ana Moita and Takeshi Hori and Hirokazu Kaji and Rui Lima and Gra{\c c}a Minas",

note = "Funding Information: Funding: This work has been supported by the projects NORTE-01-0145-FEDER-030171 (project reference PTDC/EME-SIS/30171/2017), NORTE-01-0145-FEDER-029394 (project reference PTDC/EMD-EMD/29394/2017), through the COMPETE2020, the Lisb@2020, the Programa Operacional Regional do Norte–Norte Portugal Regional Operational Programme (NORTE 2020), under the PORTUGAL 2020 Partnership Agreement through the European Regional Development Fund (FEDER) and by Funda{\c c}{\~a}o para a Ci{\^e}ncia e Tecnologia (FCT), and through FEDER and FCT, project references EXPL/EMD-EMD/0650/2021 and PTDC/EEI-EEE/2846/2021. The authors also acknowledge the partial financial support within the R&D Units Project Scope: UIDB/00319/2020, UIDB/04077/2020, UIDB/00690/2020, UIDB/04436/2020. This work was also funded by AMED-CREST Grant Number JP20gm1310001h0002. Raquel O. Rodrigues (R.O.R.) thanks FCT for her contract funding provided through 2020.03975.CEECIND. Funding Information: Acknowledgments: In{\^e}s Gon{\c c}alves (I.G.) acknowledges the PhD scholarship BD/08646/2020 attributed by FCT. Violeta Carvalho (V.C.) acknowledges the PhD scholarship UI/BD/151028/2021 attributed by FCT. Publisher Copyright: {\textcopyright} 2022 by the authors. Licensee MDPI, Basel, Switzerland.",

year = "2022",

month = feb,

day = "1",

doi = "10.3390/cancers14040935",

language = "English",

volume = "14",

journal = "Cancers",

issn = "2072-6694",

publisher = "Multidisciplinary Digital Publishing Institute (MDPI)",

number = "4",

}

TY - JOUR

T1 - Organ-on-a-Chip Platforms for Drug Screening and Delivery in Tumor Cells

T2 - A Systematic Review

AU - Gonçalves, Inês M.

AU - Carvalho, Violeta

AU - Rodrigues, Raquel O.

AU - Pinho, Diana

AU - Teixeira, Senhorinha F.C.F.

AU - Moita, Ana

AU - Hori, Takeshi

AU - Kaji, Hirokazu

AU - Lima, Rui

AU - Minas, Graça

N1 - Funding Information: Funding: This work has been supported by the projects NORTE-01-0145-FEDER-030171 (project reference PTDC/EME-SIS/30171/2017), NORTE-01-0145-FEDER-029394 (project reference PTDC/EMD-EMD/29394/2017), through the COMPETE2020, the Lisb@2020, the Programa Operacional Regional do Norte–Norte Portugal Regional Operational Programme (NORTE 2020), under the PORTUGAL 2020 Partnership Agreement through the European Regional Development Fund (FEDER) and by Fundação para a Ciência e Tecnologia (FCT), and through FEDER and FCT, project references EXPL/EMD-EMD/0650/2021 and PTDC/EEI-EEE/2846/2021. The authors also acknowledge the partial financial support within the R&D Units Project Scope: UIDB/00319/2020, UIDB/04077/2020, UIDB/00690/2020, UIDB/04436/2020. This work was also funded by AMED-CREST Grant Number JP20gm1310001h0002. Raquel O. Rodrigues (R.O.R.) thanks FCT for her contract funding provided through 2020.03975.CEECIND. Funding Information: Acknowledgments: Inês Gonçalves (I.G.) acknowledges the PhD scholarship BD/08646/2020 attributed by FCT. Violeta Carvalho (V.C.) acknowledges the PhD scholarship UI/BD/151028/2021 attributed by FCT. Publisher Copyright: © 2022 by the authors. Licensee MDPI, Basel, Switzerland.

PY - 2022/2/1

Y1 - 2022/2/1

N2 - The development of cancer models that rectify the simplicity of monolayer or static cell cultures physiologic microenvironment and, at the same time, replicate the human system more accurately than animal models has been a challenge in biomedical research. Organ-on-a-chip (OoC) devices are a solution that has been explored over the last decade. The combination of microfluidics and cell culture allows the design of a dynamic microenvironment suitable for the evaluation of treatments’ efficacy and effects, closer to the response observed in patients. This systematic review sums the studies from the last decade, where OoC with cancer cell cultures were used for drug screening assays. The studies were selected from three databases and analyzed following the research guidelines for systematic reviews proposed by PRISMA. In the selected studies, several types of cancer cells were evaluated, and the majority of treatments tested were standard chemotherapeutic drugs. Some studies reported higher drug resistance of the cultures on the OoC devices than on 2D cultures, which indicates the better resemblance to in vivo conditions of the former. Several studies also included the replication of the microvasculature or the combination of different cell cultures. The presence of vasculature can influence positively or negatively the drug efficacy since it con-tributes to a greater diffusion of the drug and also oxygen and nutrients. Co-cultures with liver cells contributed to the evaluation of the systemic toxicity of some drugs metabolites. Nevertheless, few studies used patient cells for the drug screening assays.

AB - The development of cancer models that rectify the simplicity of monolayer or static cell cultures physiologic microenvironment and, at the same time, replicate the human system more accurately than animal models has been a challenge in biomedical research. Organ-on-a-chip (OoC) devices are a solution that has been explored over the last decade. The combination of microfluidics and cell culture allows the design of a dynamic microenvironment suitable for the evaluation of treatments’ efficacy and effects, closer to the response observed in patients. This systematic review sums the studies from the last decade, where OoC with cancer cell cultures were used for drug screening assays. The studies were selected from three databases and analyzed following the research guidelines for systematic reviews proposed by PRISMA. In the selected studies, several types of cancer cells were evaluated, and the majority of treatments tested were standard chemotherapeutic drugs. Some studies reported higher drug resistance of the cultures on the OoC devices than on 2D cultures, which indicates the better resemblance to in vivo conditions of the former. Several studies also included the replication of the microvasculature or the combination of different cell cultures. The presence of vasculature can influence positively or negatively the drug efficacy since it con-tributes to a greater diffusion of the drug and also oxygen and nutrients. Co-cultures with liver cells contributed to the evaluation of the systemic toxicity of some drugs metabolites. Nevertheless, few studies used patient cells for the drug screening assays.

KW - Cancer cells

KW - Cell culture

KW - Drug delivery

KW - Drug screening

KW - Hard tissues and organs

KW - Microbioreactor

KW - Microfluidics

KW - Nanoparticles

KW - Organ-on-a-chip

KW - Organoids

UR - http://www.scopus.com/inward/record.url?scp=85124359842&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85124359842&partnerID=8YFLogxK

U2 - 10.3390/cancers14040935

DO - 10.3390/cancers14040935

M3 - Review article

AN - SCOPUS:85124359842

SN - 2072-6694

VL - 14

JO - Cancers

JF - Cancers

IS - 4

M1 - 935

ER -

Organ-on-a-Chip Platforms for Drug Screening and Delivery in Tumor Cells: A Systematic Review

Abstract

Keywords

ASJC Scopus subject areas

UN SDGs

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