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The Big Picture of Glioblastoma Malignancy: A Meta-Analysis of Glioblastoma Proteomics to Identify Altered Biological Pathways

journal contribution
posted on 2025-02-26, 20:46 authored by AKW Tribe, Melanie-Jane McConnellMelanie-Jane McConnell, Paul Teesdale-SpittlePaul Teesdale-Spittle
Glioblastoma is a highly malignant cancer with no effective treatment. It is vital to elucidate the mechanisms which drive glioblastoma in order to identify therapeutic targets. The differences in protein expression between glioblastoma, grade I-III glioma, and normal brain tissue reflect the functional alterations driving malignancy. However, proteomic analysis of glioblastoma has been hampered by the heterogeneity of glioblastoma and the variety of methodology used in its study. To reduce these inconsistencies, we performed a meta-analysis of the literature published since 2015, including 14 datasets from eight papers comparing the whole proteome of glioblastoma to normal brain or grade I-III glioma. We found that 154 proteins were commonly upregulated and 116 proteins were commonly downregulated in glioblastoma compared to normal brain. Meanwhile, 240 proteins were commonly upregulated and 125 proteins were commonly downregulated in glioblastoma compared to grade I-III glioma. Functional enrichment analysis revealed upregulation of proteins involved in mRNA splicing and the immune system and downregulation of proteins involved in synaptic signaling and glucose and glutamine metabolism. The identification of these altered biological pathways provides a basis for deeper investigation in the pursuit of an effective treatment for glioblastoma.

History

Preferred citation

Tribe, A. K. W., McConnell, M. J. & Teesdale-Spittle, P. H. (2021). The Big Picture of Glioblastoma Malignancy: A Meta-Analysis of Glioblastoma Proteomics to Identify Altered Biological Pathways. ACS Omega, 6(38), 24535-24544. https://doi.org/10.1021/acsomega.1c02991

Journal title

ACS Omega

Volume

6

Issue

38

Publication date

2021-09-28

Pagination

24535-24544

Publisher

American Chemical Society (ACS)

Publication status

Published

Online publication date

2021-09-14

ISSN

2470-1343

eISSN

2470-1343

Language

en