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Three-dimensional bioprinted glioblastoma microenvironments model cellular dependencies and immune interactions

Authors :
Jacob Schimelman
Tyler E. Miller
Benjamin F. Cravatt
Alysson R. Muotri
Shruti Bhargava
Zheng Zhong
Deobrat Dixit
Derrick Lee
Shaochen Chen
Xueyi Wan
Bingjie Sun
Michael H. Lorenzini
Qi Xie
Jing Tian
Aaron Yu
Jeremy N. Rich
Reilly L. Kidwell
Zhixin Qiu
Linjie Zhao
Ryan C. Gimple
Hui Jing
Briana C. Prager
Zhe Zhu
Jing Tang
Pengrui Wang
Pinar Mesci
Min Tang
Trevor Tam
Qiulian Wu
Source :
Cell Research, Cell research, vol 30, iss 10
Publication Year :
2019

Abstract

Brain tumors are dynamic complex ecosystems with multiple cell types. To model the brain tumor microenvironment in a reproducible and scalable system, we developed a rapid three-dimensional (3D) bioprinting method to construct clinically relevant biomimetic tissue models. In recurrent glioblastoma, macrophages/microglia prominently contribute to the tumor mass. To parse the function of macrophages in 3D, we compared the growth of glioblastoma stem cells (GSCs) alone or with astrocytes and neural precursor cells in a hyaluronic acid-rich hydrogel, with or without macrophage. Bioprinted constructs integrating macrophage recapitulate patient-derived transcriptional profiles predictive of patient survival, maintenance of stemness, invasion, and drug resistance. Whole-genome CRISPR screening with bioprinted complex systems identified unique molecular dependencies in GSCs, relative to sphere culture. Multicellular bioprinted models serve as a scalable and physiologic platform to interrogate drug sensitivity, cellular crosstalk, invasion, context-specific functional dependencies, as well as immunologic interactions in a species-matched neural environment.

Details

ISSN :
17487838
Volume :
30
Issue :
10
Database :
OpenAIRE
Journal :
Cell research
Accession number :
edsair.doi.dedup.....d4e1dd009c90fa2f5be8d89ab283f158