Functional Graphene for Peritumoral Brain Microenvironment Modulation Therapy in Glioblastoma

Author:

Chin Shan Min1,Reina Giacomo2,Chau Ngoc Do Quyen2,Chabrol Tanguy1,Wion Didier1,Bouamrani Ali1,Gay Emmanuel1,Nishina Yuta34,Bianco Alberto2ORCID,Berger François1

Affiliation:

1. Emmanuel Gay François Berger INSERM UMR1205 Brain Tech Lab Grenoble Alpes University Grenoble 38000 France

2. CNRS Immunology Immunopathology and Therapeutic Chemistry UPR3572 University of Strasbourg ISIS Strasbourg 67000 France

3. Graduate School of Natural Science and Technology Okayama University Tsushimanaka Kita‐ku Okayama 700‐8530 Japan

4. Research Core for Interdisciplinary Sciences Okayama University Tsushimanaka Kita‐ku Okayama 700‐8530 Japan

Abstract

AbstractPeritumoral brain invasion is the main target to cure glioblastoma. Chemoradiotherapy and targeted therapies fail to combat peritumoral relapse. Brain inaccessibility and tumor heterogeneity explain this failure, combined with overlooking the peritumor microenvironment. Reduce graphene oxide (rGO) provides a unique opportunity to modulate the local brain microenvironment. Multimodal graphene impacts are reported on glioblastoma cells in vitro but fail when translated in vivo because of low diffusion. This issue is solved by developing a new rGO formulation involving ultramixing during the functionalization with polyethyleneimine (PEI) leading to the formation of highly water‐stable rGO‐PEI. Wide mice brain diffusion and biocompatibility are demonstrated. Using an invasive GL261 model, an anti‐invasive effect is observed. A major unexpected modification of the peritumoral area is also observed with the neutralization of gliosis. In vitro, mechanistic investigations are performed using primary astrocytes and cytokine array. The result suggests that direct contact of rGO‐PEIUT neutralizes astrogliosis, decreasing several proinflammatory cytokines that would explain a bystander tumor anti‐invasive effect. rGO also significantly downregulates several proinvasive/protumoral cytokines at the tumor cell level. The results open the way to a new microenvironment anti‐invasive nanotherapy using a new graphene nanomaterial that is optimized for in vivo brain delivery.

Funder

Okayama University

Publisher

Wiley

Subject

Biomaterials,Biotechnology,General Materials Science,General Chemistry

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