Tumor-associated monocytes promote mesenchymal transformation through EGFR signaling in glioma

Basic information
Sample
5

Technology
10X Genomics
Omics
scRNA-seq
Source
PBMCs

Dataset ID
37652019
Platform
Illumina NovaSeq 6000
Species
Human
Disease
Glioblastoma (GB)
Age range
34 - 74
Update date
2023-09-19
Summary

The role of brain immune compartments in glioma evolution remains elusive. We profile immune cells in glioma microenvironment and the matched peripheral blood from 11 patients. Glioblastoma exhibits specific infiltration of blood-originated monocytes expressing epidermal growth factor receptor (EGFR) ligands EREG and AREG, coined as tumor-associated monocytes (TAMo). TAMo infiltration is mutually exclusive with EGFR alterations (p = 0.019), while co-occurring with mesenchymal subtype (p = 4.7 × 10−7) and marking worse prognosis (p = 0.004 and 0.032 in two cohorts). Evolutionary analysis of initial-recurrent glioma pairs and single-cell study of a multi-centric glioblastoma reveal association between elevated TAMo and glioma mesenchymal transformation. Further analyses identify FOSL2 as a TAMo master regulator and demonstrates that FOSL2-EREG/AREG-EGFR signaling axis promotes glioma invasion in vitro. Collectively, we identify TAMo in tumor microenvironment and reveal its driving role in activating EGFR signaling to shape glioma evolution.

Overall design

The GB or peripheral blood cell suspension was loaded into Chromium microfluidic chips with 3’ (v3) chemistry and barcoded with a 10× Chromium Controller (10X Genomics). RNA from the barcoded cells was subsequently reverse-transcribed and sequencing libraries constructed with reagents from a Chromium Single Cell 3’ (v3) reagent kit (10X Genomics) according to the manufacturer’s recommendations. Sequencing was performed with Illumina (NovaSeq) according to the manufacturer’s recommendations (Illumina).

Contributors

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Contact

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snRNA-Seq
Sample nameSample titleDiseaseGenderAgeSourceTreatmentTechnologyPlatformOmicsSample IDDataset IDAction
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