TMIC-06. GLIOBLASTOMA PROGRESSION IS PROMOTED BY C5AR1 SIGNALING THROUGH EMT INDUCTION, AND ITS BLOCKADE BY W54011 ATTENUATES MALIGNANT PHENOTYPES

Abstract BACKGROUND Glioblastoma multiforme (GBM) is an aggressive brain tumor with poor prognosis. Tumor mesenchymal stem-like cells (tMSLCs) in GBM tissues secrete complement component 5a (C5a), which promotes tumor malignancy. This study aimed to investigate the impact of C5a on GBM tumorspheres...

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Published in:Neuro-oncology (Charlottesville, Va.) Va.), 2023-11, Vol.25 (Supplement_5), p.v279-v279
Main Authors: Yoo, Jihwan, Oh, Yoojung, Lee, Dongkyu, Choi, Seonah, Kim, Eui-Hyun, Moon, Ju Hyung, Chang, Jong Hee, Kang, Seok-Gu
Format: Article
Language:English
Subjects:
Tumor Microenvironment
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Summary:Abstract BACKGROUND Glioblastoma multiforme (GBM) is an aggressive brain tumor with poor prognosis. Tumor mesenchymal stem-like cells (tMSLCs) in GBM tissues secrete complement component 5a (C5a), which promotes tumor malignancy. This study aimed to investigate the impact of C5a on GBM tumorspheres (GBM-TS) and to evaluate the therapeutic potential of C5a inhibition using the C5a antagonist, W54011. METHODS RNA sequencing (RNAseq) was performed on tumor tissues to identify differentiaaly expressing genes (DEG) and perform gene set enrichment analysia (GSEA) to correlate with patient survival based on C5aR1 expression. GBM-TS and tMSLCs were cultured to create a conditioned medium (CM) containing C5a, which was used to stimulate GBM-TS. The effect of C5a on GBM-TS proliferation, invasion, and stemness was determined using WST/ATP assay, 3D invasion assay, and neurosphere formation assay. Western blot and RNAseq analysis were performed to validate the results. In vivo studies were conducted using orthotopic xenograft mouse models injected with GBM-TS alone or with CM and treated with W54011. RESULTS Patients with high C5aR1 expression had a poor prognosis. Treatment with CM increased proliferation, invasion, and stemness of GBM-TS, but W54011 reversed these effects. Treatment with CM induced epithelial-messenchymal transition (EMT) in GBM TSs, whereas W54011 restored the spherical morphology and induced apoptosis. Our results were supported by transcriptome analysis and marker expression in Western blots. In the orthotopic xenograft mouse model, co-injection of GBM-TS and CM resulted in larger tumors and poorer survival, while treatment with W54011 reduced tumor size. CONCLUSIONS C5a promotes the growth, invasion, and stemness of GBM-TS, and inhibition of C5a using W54011 may have therapeutic potential for patients with high C5a expression. These results provide insight into the underlying mechanisms of GBM progression and establish a knowledge base for the clinical efficacy of W54011 in GBM treatment.
ISSN:1522-8517
1523-5866
DOI:10.1093/neuonc/noad179.1072