Development of a 3D Co-Culture System as a Cancer Model Using a Self-Assembling Peptide Scaffold
Cancer research has traditionally relied on two-dimensional (2D) cell culture, focusing mainly on cancer cells and their abnormal genetics. However, over the past decade, tumors have been accepted as complex tissues rather than a homogenous mass of proliferating cells. Consequently, cancer cells&...
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MDPI AG
2018-08-01
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| Online Access: | http://www.mdpi.com/2310-2861/4/3/65 |
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doaj-c3d2ac5f9ca04e06bef85406868495282020-11-25T00:49:45ZengMDPI AGGels2310-28612018-08-01436510.3390/gels4030065gels4030065Development of a 3D Co-Culture System as a Cancer Model Using a Self-Assembling Peptide ScaffoldNausika Betriu0Carlos E. Semino1Tissue Engineering Research Laboratory, Department of Bioengineering, IQS-School of Engineering, Ramon Llull University, 08017 Barcelona, SpainTissue Engineering Research Laboratory, Department of Bioengineering, IQS-School of Engineering, Ramon Llull University, 08017 Barcelona, SpainCancer research has traditionally relied on two-dimensional (2D) cell culture, focusing mainly on cancer cells and their abnormal genetics. However, over the past decade, tumors have been accepted as complex tissues rather than a homogenous mass of proliferating cells. Consequently, cancer cells’ behavior can only be deciphered considering the contribution of the cells existing in the tumor stroma as well as its complex microenvironment. Since the tumor microenvironment plays a critical role in tumorigenesis, it is widely accepted that culturing cells in three-dimensional (3D) scaffolds, which mimic the extracellular matrix, represents a more realistic scenario. In the present work, an in vitro 3D co-culture system based on the self-assembling peptide scaffold RAD16-I (SAPS RAD16-I) was developed as a cancer model. For that, PANC-1 cells were injected into a RAD16-I peptide scaffold containing fibroblasts, resulting in a 3D system where cancer cells were localized in a defined area within a stromal cells matrix. With this system, we were able to study the effect of three well-known pharmaceutical drugs (Gemcitabine, 5-Fluorouracil (5-FU), and 4-Methylumbelliferone (4-MU)) in a 3D context in terms of cell proliferation and survival. Moreover, we have demonstrated that the anti-cancer effect of the tested compounds can be qualitatively and quantitatively evaluated on the developed 3D co-culture system. Experimental results showed that Gemcitabine and 5-FU prevented PANC-1 cell proliferation but had a high cytotoxic effect on fibroblasts as well. 4-MU had a subtle effect on PANC-1 cells but caused high cell death on fibroblasts.http://www.mdpi.com/2310-2861/4/3/65self-assembling peptide scaffold RAD16-Ithree-dimensional cultureco-culture systemtumor microenvironment |
| collection |
DOAJ |
| language |
English |
| format |
Article |
| sources |
DOAJ |
| author |
Nausika Betriu Carlos E. Semino |
| spellingShingle |
Nausika Betriu Carlos E. Semino Development of a 3D Co-Culture System as a Cancer Model Using a Self-Assembling Peptide Scaffold Gels self-assembling peptide scaffold RAD16-I three-dimensional culture co-culture system tumor microenvironment |
| author_facet |
Nausika Betriu Carlos E. Semino |
| author_sort |
Nausika Betriu |
| title |
Development of a 3D Co-Culture System as a Cancer Model Using a Self-Assembling Peptide Scaffold |
| title_short |
Development of a 3D Co-Culture System as a Cancer Model Using a Self-Assembling Peptide Scaffold |
| title_full |
Development of a 3D Co-Culture System as a Cancer Model Using a Self-Assembling Peptide Scaffold |
| title_fullStr |
Development of a 3D Co-Culture System as a Cancer Model Using a Self-Assembling Peptide Scaffold |
| title_full_unstemmed |
Development of a 3D Co-Culture System as a Cancer Model Using a Self-Assembling Peptide Scaffold |
| title_sort |
development of a 3d co-culture system as a cancer model using a self-assembling peptide scaffold |
| publisher |
MDPI AG |
| series |
Gels |
| issn |
2310-2861 |
| publishDate |
2018-08-01 |
| description |
Cancer research has traditionally relied on two-dimensional (2D) cell culture, focusing mainly on cancer cells and their abnormal genetics. However, over the past decade, tumors have been accepted as complex tissues rather than a homogenous mass of proliferating cells. Consequently, cancer cells’ behavior can only be deciphered considering the contribution of the cells existing in the tumor stroma as well as its complex microenvironment. Since the tumor microenvironment plays a critical role in tumorigenesis, it is widely accepted that culturing cells in three-dimensional (3D) scaffolds, which mimic the extracellular matrix, represents a more realistic scenario. In the present work, an in vitro 3D co-culture system based on the self-assembling peptide scaffold RAD16-I (SAPS RAD16-I) was developed as a cancer model. For that, PANC-1 cells were injected into a RAD16-I peptide scaffold containing fibroblasts, resulting in a 3D system where cancer cells were localized in a defined area within a stromal cells matrix. With this system, we were able to study the effect of three well-known pharmaceutical drugs (Gemcitabine, 5-Fluorouracil (5-FU), and 4-Methylumbelliferone (4-MU)) in a 3D context in terms of cell proliferation and survival. Moreover, we have demonstrated that the anti-cancer effect of the tested compounds can be qualitatively and quantitatively evaluated on the developed 3D co-culture system. Experimental results showed that Gemcitabine and 5-FU prevented PANC-1 cell proliferation but had a high cytotoxic effect on fibroblasts as well. 4-MU had a subtle effect on PANC-1 cells but caused high cell death on fibroblasts. |
| topic |
self-assembling peptide scaffold RAD16-I three-dimensional culture co-culture system tumor microenvironment |
| url |
http://www.mdpi.com/2310-2861/4/3/65 |
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