Abstract

Currently, the two primary patient-derived xenograft (PDX) models of glioblastoma are established through intracranial or subcutaneous injection. In this study, a novel PDX model of glioblastoma was developed via intravitreal injection to facilitate tumor formation in a brain-mimicking microenvironment with improved visibility and fast development. Glioblastoma cells were prepared from the primary and recurrent tumor tissues of a 39-year-old female patient. To demonstrate the feasibility of intracranial tumor formation, U-87 MG and patient-derived glioblastoma cells were injected into the brain parenchyma of Balb/c nude mice. Unlike the U-87 MG cells, the patient-derived glioblastoma cells failed to form intracranial tumors until 6 weeks after tumor cell injection. In contrast, the patient-derived cells effectively formed intraocular tumors, progressing from plaques at 2 weeks to masses at 4 weeks after intravitreal injection. The in vivo tumors exhibited the same immunopositivity for human mitochondria, GFAP, vimentin, and nestin as the original tumors in the patient. Furthermore, cells isolated from the in vivo tumors also demonstrated morphology similar to that of their parental cells and immunopositivity for the same markers. Overall, a novel PDX model of glioblastoma was established via the intravitreal injection of tumor cells. This model will be an essential tool to investigate and develop novel therapeutic alternatives for the treatment of glioblastoma.

Highlights

  • Patient-derived xenograft (PDX) models of glioblastoma are based on the subcutaneous or intracranial injection of tumor cells into immunocompromised mice[1]

  • In this study, a novel PDX model of glioblastoma was established via the intravitreal injection of tumor cells

  • It is remarkable that the patient-derived glioblastoma cells that did not form intracranial tumors at 6 weeks after injection effectively formed intraocular tumors at 4 weeks

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Summary

Introduction

Patient-derived xenograft (PDX) models of glioblastoma are based on the subcutaneous or intracranial injection of tumor cells into immunocompromised mice[1]. These models have been valuable tools to investigate tumor characteristics[2,3] and the potential therapeutic efficacies of various treatment options[1,4,5,6,7,8]. Via subcutaneous injection, PDX tumors develop rapidly but are In this context, it is remarkable that the retina in the eye and the brain share several neurovascular characteristics in common. Other cellular components of the tumor microenvironment of glioblastoma, including microglia and immune cells, are quite similar between the brain and retina[15,16,17]

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