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Cytomegalovirus promotes murine glioblastoma growth via pericyte recruitment and angiogenesis
Harald Krenzlin, Prajna Behera, Viola Lorenz, Carmela Passaro, Mykola Zdioruk, Michal O. Nowicki, Korneel Grauwet, Hong Zhang, Magdalena Skubal, Hirotaka Ito, Rachel Zane, Michael Gutknecht, Marion B. Griessl, Franz Ricklefs, Lai Ding, Sharon Peled, Arun Rooj, C. David James, Charles S. Cobbs, Charles H. Cook, E. Antonio Chiocca, Sean E. Lawler
Harald Krenzlin, Prajna Behera, Viola Lorenz, Carmela Passaro, Mykola Zdioruk, Michal O. Nowicki, Korneel Grauwet, Hong Zhang, Magdalena Skubal, Hirotaka Ito, Rachel Zane, Michael Gutknecht, Marion B. Griessl, Franz Ricklefs, Lai Ding, Sharon Peled, Arun Rooj, C. David James, Charles S. Cobbs, Charles H. Cook, E. Antonio Chiocca, Sean E. Lawler
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Research Article Oncology Virology

Cytomegalovirus promotes murine glioblastoma growth via pericyte recruitment and angiogenesis

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Abstract

Cytomegalovirus (CMV) has been implicated in glioblastoma (GBM); however, a mechanistic connection in vivo has not been established. The purpose of this study is to characterize the effects of murine CMV (MCMV) on GBM growth in murine models. Syngeneic GBM models were established in mice perinatally infected with MCMV. We found that tumor growth was markedly enhanced in MCMV+ mice, with a significant reduction in overall survival compared with that of controls (P < 0.001). We observed increased angiogenesis and tumor blood flow in MCMV+ mice. MCMV reactivation was observed in intratumoral perivascular pericytes and tumor cells in mouse and human GBM specimens, and pericyte coverage of tumor vasculature was strikingly augmented in MCMV+ mice. We identified PDGF-D as a CMV-induced factor essential for pericyte recruitment, angiogenesis, and tumor growth. The antiviral drug cidofovir improved survival in MCMV+ mice, inhibiting MCMV reactivation, PDGF-D expression, pericyte recruitment, and tumor angiogenesis. These data show that MCMV potentiates GBM growth in vivo by increased pericyte recruitment and angiogenesis due to alterations in the secretome of CMV-infected cells. Our model provides evidence for a role of CMV in GBM growth and supports the application of antiviral approaches for GBM therapy.

Authors

Harald Krenzlin, Prajna Behera, Viola Lorenz, Carmela Passaro, Mykola Zdioruk, Michal O. Nowicki, Korneel Grauwet, Hong Zhang, Magdalena Skubal, Hirotaka Ito, Rachel Zane, Michael Gutknecht, Marion B. Griessl, Franz Ricklefs, Lai Ding, Sharon Peled, Arun Rooj, C. David James, Charles S. Cobbs, Charles H. Cook, E. Antonio Chiocca, Sean E. Lawler

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Figure 3

CMV associates with vascular pericytes in GBM.

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CMV associates with vascular pericytes in GBM.
(A) CMV (green, Virusys C...
(A) CMV (green, Virusys CA150-1 antibody; red, Virusys CA003-100 antibody) immunofluorescence staining in brain sections from animals at the end point of survival studies. DAPI-stained nuclei are shown in blue. Scale bar: 50 μm. (B) Real-time qPCR analysis of MCMV IE1/m123 mRNA levels in GL261Luc2 tumors from MCMV+ and naive mice. n = 3. Box extends from 25th to 75th percentile, and median is indicated by horizontal line. Whiskers represent maximum and minimum values. *P < 0.05; ***P < 0.005, Holm-Šídák test. (C) CMV (red, Virusys CA003-100), CD31 (green), and NG2 (green) immunofluorescence in tumor sections from MCMV+ mice. DAPI-stained nuclei are shown in blue. Scale bar: 50 μm. (D) CD31 (red), NG2 (green), and nuclei (blue) immunofluorescence in tumors from MCMV+ mice. Scale bar: 50 μm. (E) NG2 fluorescence intensity in 12 independent fields of view from murine GBMs. n = 3. Box extends from 25th to 75th percentile, and median is indicated by horizontal line. Whiskers represent maximum and minimum values. Scale bar: 50 μm. ***P < 0.005, Student’s t test. (F) CMV (red, Virusys CA003-100), CD31 (green), and NG2 (green) immunostaining immunofluorescence in human GBM. Scale bar: 50 μm. Pearson’s rank colocalization. n = 3. Box extends from 25th to 75th percentile, and median is indicated by horizontal line. Whiskers represent maximum and minimum values.

Copyright © 2026 American Society for Clinical Investigation
ISSN: 0021-9738 (print), 1558-8238 (online)

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