BRAF V600E in a Preclinical Model of Pleomorphic Xanthoastrocytoma: Analysis of the Tumor Microenvironment and Immune Cell Infiltration Dynamics

Overview

Journal Mol Ther Oncol

Date 2024 May 24

PMID 38784952

Authors

Alessandro Canella

Matthew Nazzaro

Mykyta Artomov

Lakshmi Prakruthi Rao Venkata

Diana Thomas

Justin Lyberger

Aleksandr Ukhatov

Yao Lulu Xing

Katherine Miller

Gregory Behbehani

Nduka M Amankulor

Claudia Katharina Petritsch

Prajwal Rajappa

Affiliations

Soon will be listed here.

Abstract

Low-grade glioma (LGG) is the most common brain tumor affecting pediatric patients (pLGG) and BRAF mutations constitute the most frequent genetic alterations. Within the spectrum of pLGGs, approximately 70%-80% of pediatric patients diagnosed with transforming pleomorphic xanthoastrocytoma (PXA) harbor the BRAF V600E mutation. However, the impact of glioma BRAF V600E cell regulation of tumor-infiltrating immune cells and their contribution to tumor progression remains unclear. Moreover, the efficacy of BRAF inhibitors in treating pLGGs is limited compared with their impact on BRAF-mutated melanoma. Here we report a novel immunocompetent RCAS-BRAF V600E murine glioma model. Pathological assessment indicates this model seems to be consistent with diffuse gliomas and morphological features of PXA. Our investigations revealed distinct immune cell signatures associated with increased trafficking and activation within the tumor microenvironment (TME). Intriguingly, immune system activation within the TME also generated a pronounced inflammatory response associated with dysfunctional CD8 T cells, increased presence of immunosuppressive myeloid cells and regulatory T cells. Further, our data suggests tumor-induced inflammatory processes, such as cytokine storm. These findings suggest a complex interplay between tumor progression and the robust inflammatory response within the TME in preclinical BRAF V600E LGGs, which may significantly influence animal survival.

Citing Articles

Primary murine high-grade glioma cells derived from RCAS/tv-a diffuse glioma model reprogram naive T cells into immunosuppressive regulatory T lymphocytes.

Canella A, Artomov M, Ukhatov A, Rajendran S, Perez P, Saini U Mol Ther Oncol. 2024; 32(3):200861.

PMID: 39328291 PMC: 11426037. DOI: 10.1016/j.omton.2024.200861.

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