Isolation and characterization of patient-derived CNS metastasis-associated stromal cell lines

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作者
Ben Yi Tew
Christophe Legendre
Gerald C. Gooden
Kyle N. Johnson
Rae Anne Martinez
Jeff Kiefer
Mark Bernstein
Jennifer Glen
Loren Butry
Aleksander Hinek
Steven A. Toms
Bodour Salhia
机构
[1] University of Southern California,Department of Translational Genomics, Keck School of Medicine, Norris Comprehensive Cancer Center
[2] Translational Genomics Research Institute,Division of Neurosurgery
[3] University Health Network,Peter Gilgan Centre for Research and Learning
[4] Hospital for Sickkids,Department of Neurosurgery
[5] Geisinger Health System,Department of Neurosurgery
[6] Lifespan Health System and Warren Alpert School of Medicine,undefined
[7] Brown University,undefined
来源
Oncogene | 2019年 / 38卷
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摘要
The functional role of human derived stromal cells in the tumor microenviornment of CNS metastases (CM) remain understudied. The purpose of the current study was to isolate and characterize stromal cells of the tumor microenvironment in CM. Four different patient-derived cell lines (PDCs) of stromal and one PDC of tumorigenic origin were generated from breast or lung CM. PDCs were analyzed by DNA/RNA sequencing, DNA methylation profiling, and immunophenotypic assays. The stromal derived PDCs were termed CNS metastasis-associated stromal cells (cMASCs). Functional analysis of cMASCs was tested by co-implanting them with tumorigenic cells in mice. cMASCs displayed normal genotypes compared with tumorigenic cell lines. RNA-seq and DNA methylation analyses demonstrated that cMASCs highly resembled each other, suggesting a common cell of origin. Additionally, cMASCs revealed gene expression signatures associated with cancer associated fibroblasts (CAFs), epithelial to mesenchymal transition, mesenchymal stem cells and expressed high levels of collagen. Functionally, cMASCs restricted tumor growth, and induced desmoplasia in vivo, suggesting that cMASCs may promote a protective host response to impede tumor growth. In summary, we demonstrated the isolation, molecular characterization and functional role of human derived cMASCs, a subpopulation of cells in the microenvironment of CM that have tumor inhibitory functions.
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页码:4002 / 4014
页数:12
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