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Systemic miRNA-7 delivery inhibits tumor angiogenesis and growth in murine xenograft glioblastoma

Authors :
Maaike van Berkel
Francesco Cerisoli
Raymond M. Schiffelers
Paula I. van Noort
Mark Verheul
Judy R. van Beijnum
Yijia Liu
Rick Jan van Haastert
Gert Storm
Martin C. Woodle
Grégoire Pierre André Prevost
Roel Q.J. Schaapveld
Enrico Mastrobattista
Ebel H. E. Pieters
Arjan W. Griffioen
Puthupparampil V. Scaria
Meriem Bourajjaj
Afrouz Yousefi
Eugene Berezikov
Negar Babae
Edwin Cuppen
Hubrecht Institute for Developmental Biology and Stem Cell Research
Biomaterials Science and Technology
Faculty of Science and Technology
Medical oncology laboratory
CCA - Innovative therapy
Source :
Scopus-Elsevier, Oncotarget, 5(16), 6687-700. Impact Journals, Oncotarget, 5(16), 6687. Impact Journals, Babae, N, Bourajjaj, M, Liu, Y, van Beijnum, J R, Cerisoli, F, Scaria, P V, Verheul, M, van Berkel, M P A, Pieters, E H E, van Haastert, R J, Yousefi, A, Mastrobattista, E, Storm, G, Berezikov, E, Cuppen, E, Woodle, M, Schaapveld, R Q J, Prevost, G P, Griffioen, A W, van Noort, P I & Schiffelers, R M 2014, ' Systemic miRNA-7 delivery inhibits tumor angiogenesis and growth in murine xenograft glioblastoma ', Oncotarget, vol. 5, no. 16, pp. 6687-6700 . https://doi.org/10.18632/oncotarget.2235, Oncotarget, 5(16), 6687-6700. Impact Journals, Oncotarget

Abstract

Tumor-angiogenesis is the multi-factorial process of sprouting of endothelial cells (EC) into micro-vessels to provide tumor cells with nutrients and oxygen. To explore miRNAs as therapeutic angiogenesis-inhibitors, we performed a functional screen to identify miRNAs that are able to decrease EC viability. We identified miRNA-7 (miR-7) as a potent negative regulator of angiogenesis. Introduction of miR-7 in EC resulted in strongly reduced cell viability, tube formation, sprouting and migration. Application of miR-7 in the chick chorioallantoic membrane assay led to a profound reduction of vascularization, similar to anti-angiogenic drug sunitinib. Local administration of miR-7 in an in vivo murine neuroblastoma tumor model significantly inhibited angiogenesis and tumor growth. Finally, systemic administration of miR-7 using a novel integrin-targeted biodegradable polymeric nanoparticles that targets both EC and tumor cells, strongly reduced angiogenesis and tumor proliferation in mice with human glioblastoma xenografts. Transcriptome analysis of miR-7 transfected EC in combination with in silico target prediction resulted in the identification of OGT as novel target gene of miR-7. Our study provides a comprehensive validation of miR-7 as novel anti-angiogenic therapeutic miRNA that can be systemically delivered to both EC and tumor cells and offers promise for miR-7 as novel anti-tumor therapeutic.

Details

ISSN :
19492553
Database :
OpenAIRE
Journal :
Scopus-Elsevier, Oncotarget, 5(16), 6687-700. Impact Journals, Oncotarget, 5(16), 6687. Impact Journals, Babae, N, Bourajjaj, M, Liu, Y, van Beijnum, J R, Cerisoli, F, Scaria, P V, Verheul, M, van Berkel, M P A, Pieters, E H E, van Haastert, R J, Yousefi, A, Mastrobattista, E, Storm, G, Berezikov, E, Cuppen, E, Woodle, M, Schaapveld, R Q J, Prevost, G P, Griffioen, A W, van Noort, P I & Schiffelers, R M 2014, ' Systemic miRNA-7 delivery inhibits tumor angiogenesis and growth in murine xenograft glioblastoma ', Oncotarget, vol. 5, no. 16, pp. 6687-6700 . https://doi.org/10.18632/oncotarget.2235, Oncotarget, 5(16), 6687-6700. Impact Journals, Oncotarget
Accession number :
edsair.doi.dedup.....0c255cfa43fb16310d4f1f95a0380ba4
Full Text :
https://doi.org/10.18632/oncotarget.2235