SIRPB1 regulates inflammatory factor expression in the glioma microenvironment via SYK: functional and bioinformatics insights

Ren Geng; Yao Zhao; Wanzhen Xu; Xiaoshan Ma; Yining Jiang; Xuefei Han; Liyan Zhao; Yunqian Li

doi:10.1186/s12967-024-05149-z

Journal of Translational Medicine (Apr 2024)

SIRPB1 regulates inflammatory factor expression in the glioma microenvironment via SYK: functional and bioinformatics insights

Ren Geng,
Yao Zhao,
Wanzhen Xu,
Xiaoshan Ma,
Yining Jiang,
Xuefei Han,
Liyan Zhao,
Yunqian Li

Affiliations

Ren Geng: Department of Neurosurgery, First Hospital of Jilin University
Yao Zhao: Department of Neurosurgery, First Hospital of Jilin University
Wanzhen Xu: Department of Neurosurgery, Qilu Hospital of Shandong University Dezhou Hospital
Xiaoshan Ma: Department of Neurosurgery, First Hospital of Jilin University
Yining Jiang: Department of Neurosurgery, First Hospital of Jilin University
Xuefei Han: Department of Neurosurgery, First Hospital of Jilin University
Liyan Zhao: Department of Blood Transfusion, Second Hospital of Jilin University
Yunqian Li: Department of Neurosurgery, First Hospital of Jilin University

DOI: https://doi.org/10.1186/s12967-024-05149-z
Journal volume & issue: Vol. 22, no. 1
pp. 1 – 19

Abstract

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Abstract Background SIRPB1 expression is upregulated in various tumor types, including gliomas, and is known to contribute to tumor progression; nevertheless, its function in the immune milieu of gliomas is still mainly unknown. Methods This study, we analyzed 1152 normal samples from the GTEx database and 670 glioma samples from the TCGA database to investigate the relationship between the expression of SIRPB1 and clinicopathological features. Moreover, SIRPB1 gene knockout THP-1 cell lines were constructed using CRISPR/Cas9 and were induced into a co-culture of macrophages and glioma cells in vitro to learn more about the role of SIRPB1 in the glioma immune milieu. Lastly, we established a prognostic model to predict the effect of SIRPB1 on prognosis. Results Significantly higher levels of SIRPB1 expression were found in gliomas, which had an adverse effect on the immune milieu and correlated poorly with patient survival. SIRPB1 activation with certain antibodies results in SYK phosphorylation and the subsequent activation of calcium, MAPK, and NF-κB signaling pathways. This phenomenon is primarily observed in myeloid-derived cells as opposed to glioma cells. In vitro co-culture demonstrated that macrophages with SIRPB1 knockout showed decreased IL1RA, CCL2, and IL-8, which were recovered upon ectopic expression of SIRPB1 but reduced again following treatment with SYK inhibitor GS9973. Critically, a lower overall survival rate was linked to increased SIRPB1 expression. Making use of SIRPB1 expression along with additional clinicopathological variables, we established a nomogram that showed a high degree of prediction accuracy. Conclusions Our study demonstrates that glioma cells can be activated by macrophages via SIRPB1, subsequently reprogramming the TME, suggesting that SIRPB1 could serve as a promising therapeutic target for gliomas.

Published in Journal of Translational Medicine

ISSN: 1479-5876 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine
Website: https://translational-medicine.biomedcentral.com/

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