A patient-designed tissue-engineered model of the infiltrative glioblastoma microenvironment

Author:

Cornelison R. C.ORCID,Yuan J. X.,Tate K. M.,Petrosky A.,Beeghly G. F.ORCID,Bloomfield M.ORCID,Schwager S. C.,Berr A. L.,Stine C. A.ORCID,Cimini D.ORCID,Bafakih F. F.,Mandell J. W.,Purow B. W.,Horton B. J.,Munson J. M.ORCID

Abstract

AbstractGlioblastoma is an aggressive brain cancer characterized by diffuse infiltration. Infiltrated glioma cells persist in the brain post-resection where they interact with glial cells and experience interstitial fluid flow. We use patient-derived glioma stem cells and human glial cells (i.e., astrocytes and microglia) to create a four-component 3D model of this environment informed by resected patient tumors. We examine metrics for invasion, proliferation, and putative stemness in the context of glial cells, fluid forces, and chemotherapies. While the responses are heterogeneous across seven patient-derived lines, interstitial flow significantly increases glioma cell proliferation and stemness while glial cells affect invasion and stemness, potentially related to CCL2 expression and differential activation. In a screen of six drugs, we find in vitro expression of putative stemness marker CD71, but not viability at drug IC50, to predict murine xenograft survival. We posit this patient-informed, infiltrative tumor model as a novel advance toward precision medicine in glioblastoma treatment.

Funder

U.S. Department of Health & Human Services | NIH | National Cancer Institute

Wallace H. Coulter Foundation

Ben and Catherine Ivy Foundation

University of Virginia Harrison Undergraduate Research Award

National Science Foundation

Publisher

Springer Science and Business Media LLC

Subject

Cancer Research,Oncology

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