Journal
ACS APPLIED MATERIALS & INTERFACES
Volume 14, Issue 31, Pages 35344-35356Publisher
AMER CHEMICAL SOC
DOI: 10.1021/acsami.2c06658
Keywords
3D bioprinting; tumor model; cell fusion; glioma stem cells; mesenchymal stem cells
Funding
- Anhui Provincial Natural Science Foundation [2208085QC81, 2208085MH251]
- Anhui Medical University Scientific Research Fund [2021xkj131]
- Research Fund of the Co-construction Project of Anhui Medical University and Affiliated Hospital [2021lcxk017]
- Basic and Clinical Cooperative Research and Promotion Program of Anhui Medical University [2021xkjT028]
- Anhui Medical University [1406012201]
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Cell fusion between GSCs and MSCs in 3D-bioprinted models promotes the progression of glioma by enhancing the malignant properties of the fused cells.
The interaction between glioma stem cells (GSCs) and mesenchymal stem cells (MSCs) in the glioma microenvironment is considered to be an important factor in promoting tumor progression, but the mechanism is still not fully elucidated. To further elucidate the interaction between GSCs and MSCs, two 3D-bioprinted tumor models (low-temperature molding and coaxial bioprinting) were used to simulate the tumor growth microenvironment. Cell fusion between GSCs and MSCs was found by the method of Cre-LoxP switch gene and RFP/GFP dual-color fluorescence tracing. The fused cells coexpressed biomarkers of GSCs and MSCs, showing stronger proliferation, cloning, and invasion abilities than GSCs and MSCs. In addition, the fused cells have stronger tumorigenic properties in nude mice, showing the pathological features of malignant tumors. In conclusion, GSCs and MSCs undergo cell fusion in 3D-bioprinted models, and the fused cells have a higher degree of malignancy than parental cells, which promotes the progression of glioma.
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