Abstract

Glioblastoma (GBM) is the most aggressive type of brain tumor. In this context, animal models represent excellent tools for the early detection and longitudinal mapping of neuronal dysfunction, that are critical in the preclinical validation of new therapeutic strategies. In a mouse glioma model, we developed sensitive behavioral readouts that allow early recognizing and following neurological symptoms. We injected GL261 cells into the primary motor cortex of syngenic mice and we used a battery of behavioral tests to longitudinally monitor the dysfunction induced by tumor growth. Grip strength test revealed an early onset of functional deficit associated to the glioma growth, with a significant forelimb weakness appearing 9 days after tumor inoculation. A later deficit was observed in the rotarod and in the grid walk tasks. Using this model, we found reduced tumor growth and maintenance of behavioral functions following treatment with Cytotoxic Necrotizing Factor 1 (CNF1) at a symptomatic stage. Our data provide a detailed and precise examination of how tumor growth reverberates on the behavioral functions of glioma-bearing mice, providing normative data for the study of therapeutic strategies for glioma treatment. The reduced tumor volume and robust functional sparing observed in CNF1-treated, glioma-bearing mice strengthen the notion that CNF1 delivery is a promising strategy for glioma therapy.

Highlights

  • Adult (age > postnatal day 60) C57BL/6J mice were used for this study. Animals were bred in our animal facility and housed in a 12 hours light/dark cycle, with food and water available ad libitum

  • Adult C57BL/6J mice were used for this study

  • To exclude any influence of circadian rhythms on behavior, all tests were performed during the same time interval each day (2:00– 5:00 pm; light phase)

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Summary

Introduction

Adult (age > postnatal day 60) C57BL/6J mice were used for this study. Animals were bred in our animal facility and housed in a 12 hours light/dark cycle, with food and water available ad libitum. Mice were tested in three different motor behavioral tasks, i. We compared glioma-bearing mice with control naïve animals in order to characterize the motor GBM model.

Results
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