Pathogenesis of peritumoral hyperexcitability in an immunocompetent CRISPR-based glioblastoma model
Asante Hatcher, … , Benjamin Deneen, Jeffrey L. Noebels
Asante Hatcher, … , Benjamin Deneen, Jeffrey L. Noebels
Published April 6, 2020
Citation Information: J Clin Invest. 2020;130(5):2286-2300. https://doi.org/10.1172/JCI133316.
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Pathogenesis of peritumoral hyperexcitability in an immunocompetent CRISPR-based glioblastoma model

Abstract

Seizures often herald the clinical appearance of gliomas or appear at later stages. Dissecting their precise evolution and cellular pathogenesis in brain malignancies could inform the development of staged therapies for these highly pharmaco-resistant epilepsies. Studies in immunodeficient xenograft models have identified local interneuron loss and excess glial glutamate release as chief contributors to network disinhibition, but how hyperexcitability in the peritumoral microenvironment evolves in an immunocompetent brain is unclear. We generated gliomas in WT mice via in utero deletion of key tumor suppressor genes and serially monitored cortical epileptogenesis during tumor infiltration with in vivo electrophysiology and GCAMP7 calcium imaging, revealing a reproducible progression from hyperexcitability to convulsive seizures. Long before seizures, coincident with loss of inhibitory cells and their protective scaffolding, gain of glial glutamate antiporter xCT expression, and reactive astrocytosis, we detected local Iba1+ microglial inflammation that intensified and later extended far beyond tumor boundaries. Hitherto unrecognized episodes of cortical spreading depolarization that arose frequently from the peritumoral region may provide a mechanism for transient neurological deficits. Early blockade of glial xCT activity inhibited later seizures, and genomic reduction of host brain excitability by deleting MapT suppressed molecular markers of epileptogenesis and seizures. Our studies confirmed xenograft tumor–driven pathobiology and revealed early and late components of tumor-related epileptogenesis in a genetically tractable, immunocompetent mouse model of glioma, allowing the complex dissection of tumor versus host pathogenic seizure mechanisms.

Authors

Asante Hatcher, Kwanha Yu, Jochen Meyer, Isamu Aiba, Benjamin Deneen, Jeffrey L. Noebels

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Figure 1

IUE tumor mice exhibited progressive cortical hyperexcitability and generalized tonic-clonic seizures during GBM invasion of the neocortex.

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IUE tumor mice exhibited progressive cortical hyperexcitability and gene...
(A) Embryos were electroporated with 3 defined tumor gene variants at E16.5. Timeline shows steps in EEG monitoring protocol. GFP+ fluorescence in whole brain reveals typical end-stage brain tumor. LV, left ventricle; NC, neocortex. (B) Representative sections show GFP+ tumor growth at P35 (before onset of EEG abnormalities), P45 to P55 (onset of cortical spiking activity), and P60 to P80 (behavioral seizures, late-stage tumor). (C) Representative bilateral frontal and parietal EEG traces during tumor growth. EEG shows normal activity until P35, vigorous interictal spike activity during the early stage of tumor emergence (P45–P55), and convulsive seizures (generalized tonic-clonic) during the late stage (P60–P80). Rarely, generalized seizures occurred before P55, and spikes may emerge before P45, possibly due to asymmetric tumor invasion. GTCS, generalized tonic-clonic seizures; LF, left frontal lobe; RF, right frontal lobe; LP, left parietal lobe; RF, right parietal lobe. (D) Prolonged DC monitoring of cortical surface slow potentials revealed normal signal at P35 (left); spontaneous episodes of unilateral SD emerged at the onset of hyperexcitability and can be recurrent events (denoted by arrows; center), or occur postictally in mice experiencing generalized seizure activity (arrow, right) at late disease stage.