Litcius/Paper detail

Interferon-γ resistance and immune evasion in glioma develop via Notch-regulated co-evolution of malignant and immune cells

Elena Parmigiani, Robert Ivánek, Chiara Rolando, Katrin Hafen, Gleb Turchinovich, F. Lehmann, Alexandra Lehmkuhl Gerber, Šime Brkić, Stephan Frank, Sara C. Meyer, Hiroaki Wakimoto, Murat Günel, Angeliki Louvi, Luigi Mariani, Daniela Finke, Georg A. Holländer, Gregor Hütter, Roxane Tussiwand, Verdon Taylor, Claudio Giachino

2022Developmental Cell41 citationsDOIOpen Access PDF

Abstract

Immune surveillance is critical to prevent tumorigenesis. Gliomas evade immune attack, but the underlying mechanisms remain poorly understood. We show that glioma cells can sustain growth independent of immune system constraint by reducing Notch signaling. Loss of Notch activity in a mouse model of glioma impairs MHC-I and cytokine expression and curtails the recruitment of anti-tumor immune cell populations in favor of immunosuppressive tumor-associated microglia/macrophages (TAMs). Depletion of T cells simulates Notch inhibition and facilitates tumor initiation. Furthermore, Notch-depleted glioma cells acquire resistance to interferon-γ and TAMs re-educating therapy. Decreased interferon response and cytokine expression by human and mouse glioma cells correlate with low Notch activity. These effects are paralleled by upregulation of oncogenes and downregulation of quiescence genes. Hence, suppression of Notch signaling enables gliomas to evade immune surveillance and increases aggressiveness. Our findings provide insights into how brain tumor cells shape their microenvironment to evade immune niche control.

Topics & Concepts

BiologyImmune systemGliomaNotch signaling pathwayDownregulation and upregulationCancer researchMicrogliaCytokineInterferonImmunologyTumor microenvironmentImmunotherapyCell biologySignal transductionInflammationGeneGeneticsNeuroinflammation and Neurodegeneration MechanismsImmune cells in cancerGlioma Diagnosis and Treatment