Hacking macrophage-associated immunosuppression for regulating glioblastoma angiogenesis

Xin Cui; Renee-Tyler Tan Morales; Weiyi Qian; Haoyu Wang; Jean-Pierre Gagner; Igor Dolgalev; Dimitris Placantonakis; David Zagzag; Luisa Cimmino; Matija Snuderl; Raymond H W Lam; Weiqiang Chen

doi:10.1016/j.biomaterials.2018.01.053

Hacking macrophage-associated immunosuppression for regulating glioblastoma angiogenesis

Biomaterials. 2018 Apr:161:164-178. doi: 10.1016/j.biomaterials.2018.01.053. Epub 2018 Feb 3.

Authors

Affiliations

¹ Department of Mechanical and Aerospace Engineering, New York University, Brooklyn, NY 11201, USA.
² Department of Pathology, New York University School of Medicine, New York, NY 10016, USA.
³ Department of Neurosurgery, New York University School of Medicine, New York, NY 10016, USA.
⁴ Department of Pathology, New York University School of Medicine, New York, NY 10016, USA; Department of Neurosurgery, New York University School of Medicine, New York, NY 10016, USA.
⁵ Department of Mechanical and Biomedical Engineering, City University of Hong Kong, Hong Kong. Electronic address: rhwlam@cityu.edu.hk.
⁶ Department of Mechanical and Aerospace Engineering, New York University, Brooklyn, NY 11201, USA. Electronic address: wchen@nyu.edu.

Abstract

Glioblastoma (GBM) is the most lethal primary adult brain tumor and its pathology is hallmarked by distorted neovascularization, diffuse tumor-associated macrophage infiltration, and potent immunosuppression. Reconstituting organotypic tumor angiogenesis models with biomimetic cell heterogeneity and interactions, pro-/anti-inflammatory milieu and extracellular matrix (ECM) mechanics is critical for preclinical anti-angiogenic therapeutic screening. However, current in vitro systems do not accurately mirror in vivo human brain tumor microenvironment. Here, we engineered a three-dimensional (3D), microfluidic angiogenesis model with controllable and biomimetic immunosuppressive conditions, immune-vascular and cell-matrix interactions. We demonstrate in vitro, GL261 and CT-2A GBM-like tumors steer macrophage polarization towards a M2-like phenotype for fostering an immunosuppressive and proangiogenic niche, which is consistent with human brain tumors. We distinguished that GBM and M2-like immunosuppressive macrophages promote angiogenesis, while M1-like pro-inflammatory macrophages suppress angiogenesis, which we coin "inflammation-driven angiogenesis." We observed soluble immunosuppressive cytokines, predominantly TGF-β1, and surface integrin (α_vβ₃) endothelial-macrophage interactions are required in inflammation-driven angiogenesis. We demonstrated tuning cell-adhesion receptors using an integrin (α_vβ₃)-specific collagen hydrogel regulated inflammation-driven angiogenesis through Src-PI3K-YAP signaling, highlighting the importance of altered cell-ECM interactions in inflammation. To validate the preclinical applications of our 3D organoid model and mechanistic findings of inflammation-driven angiogenesis, we screened a novel dual integrin (α_vβ₃) and cytokine receptor (TGFβ-R1) blockade that suppresses GBM tumor neovascularization by simultaneously targeting macrophage-associated immunosuppression, endothelial-macrophage interactions, and altered ECM. Hence, we provide an interactive and controllable GBM tumor microenvironment and highlight the importance of macrophage-associated immunosuppression in GBM angiogenesis, paving a new direction of screening novel anti-angiogenic therapies.

Keywords: Angiogenesis; ECM; Endothelial-macrophage interaction; Glioblastoma.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Brain Neoplasms / immunology*
Brain Neoplasms / metabolism*
Cell Line, Tumor
Extracellular Matrix / metabolism
Glioblastoma / immunology*
Glioblastoma / metabolism*
Macrophages / immunology
Macrophages / metabolism*
Mice
Microscopy, Confocal
Neovascularization, Pathologic / immunology
Neovascularization, Pathologic / metabolism
RAW 264.7 Cells
Signal Transduction / physiology

Abstract

Publication types

MeSH terms

Grants and funding