Investigating the impact of regulatory B cells and regulatory B cell-related genes on bladder cancer progression and immunotherapeutic sensitivity

Regulatory B cells (Bregs), a specialized subset of B cells that modulate immune responses and maintain immune tolerance in malignant tumors, have not been extensively investigated in the context of bladder cancer (BLCA). This study aims to elucidate the roles of Bregs and Breg-related genes in BLCA...

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Veröffentlicht in:Journal of experimental & clinical cancer research 2024-04, Vol.43 (1), p.101-101, Article 101
Hauptverfasser: Zhou, Jiawei, Zhou, Ranran, Zhu, Yuanchao, Deng, Shikai, Muhuitijiang, Bahaerguli, Li, Chengyao, Shi, Xiaojun, Zhang, Ling, Tan, Wanlong
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Sprache:eng
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Zusammenfassung:Regulatory B cells (Bregs), a specialized subset of B cells that modulate immune responses and maintain immune tolerance in malignant tumors, have not been extensively investigated in the context of bladder cancer (BLCA). This study aims to elucidate the roles of Bregs and Breg-related genes in BLCA. We assessed Breg infiltration levels in 34 pairs of BLCA and corresponding paracancerous tissues using immunohistochemical staining. We conducted transwell and wound healing assays to evaluate the impact of Bregs on the malignant phenotype of SW780 and T24 cells. Breg-related genes were identified through gene sets and transcriptional analysis. The TCGA-BLCA cohort served as the training set, while the IMvigor210 and 5 GEO cohorts were used as external validation sets. We employed LASSO regression and random forest for feature selection and developed a risk signature using Cox regression. Primary validation of the risk signature was performed through immunohistochemical staining and RT-qPCR experiments using the 34 local BLCA samples. Additionally, we employed transfection assays and flow cytometry to investigate Breg expansion ability and immunosuppressive functions. Breg levels in BLCA tissues were significantly elevated compared to paracancerous tissues (P 
ISSN:1756-9966
0392-9078
1756-9966
DOI:10.1186/s13046-024-03017-8