Unveiling the dynamics of B lymphocytes in systemic lupus erythematosus patients treated with belimumab through longitudinal single-cell RNA sequencing
- Authors
- Bang, So-Young; Joh, Christine Suh-Yun; Itamiya, Takahiro; Jeong, Soyoung; Lee, Jung-Ho; Kwon, Haeyoon; Jin, Hyunjin; Jung, Jaewon; Chung, Hyeyeon; Lee, Brian H.; Gong, Jeong-Ryul; Ishigaki, Kazuyoshi; Fujio, Keishi; Bae, Sang-Cheol; Kim, Hyun Je; Lee, Hye-Soon
- Issue Date
- Apr-2025
- Publisher
- Oxford University Press
- Keywords
- systemic lupus erythematosus; single-cell RNA sequencing; transcriptomics; biologics; anti-BAFF therapy; B lymphocyte
- Citation
- Rheumatology, v.64, no.4, pp 2220 - 2226
- Pages
- 7
- Indexed
- SCIE
SCOPUS
- Journal Title
- Rheumatology
- Volume
- 64
- Number
- 4
- Start Page
- 2220
- End Page
- 2226
- URI
- https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/211797
- DOI
- 10.1093/rheumatology/keae364
- ISSN
- 1462-0324
1462-0332
- Abstract
- Objectives: Unravelling the mechanisms underlying treatment response for targeted therapeutics in systemic lupus erythematosus (SLE) patients is challenging due to the limited understanding of diverse responses of circulating immune cells, particularly B cells. We investigated B lymphocyte dynamics during anti-BAFF treatment, utilizing longitudinal single-cell transcriptome data. Methods: We conducted single-cell RNA sequencing on peripheral blood mononuclear cells (PBMCs) in four Korean SLE patients before and after belimumab treatment at the following time points: 2 weeks, 1, 3, 6 and 12 months. Results: Analysing over 73 000 PBMCs, we identified eight distinct subsets of B cells and plasmablasts and analysed dynamic changes within these cell subsets: initial declines in naïve and transitional B cells followed by an increase at 3 months, contrasted by an initial increase and subsequent decrease in memory B cells by the third month. Meanwhile, plasmablasts exhibited a consistent decline throughout the treatment. B cell activation pathways, specifically in naïve and memory B cells, were downregulated during the third and sixth months. These findings were validated at the protein level throughout the first 4 weeks of treatment using flow cytometry. Comparative analysis with bulk transcriptome data from 22 Japanese SLE patients showed increased NR4A1 expression 6 months post-belimumab treatment, indicating its role in restricting self-reactive B cells, thereby contributing to the biological responses of anti-BAFF treatment. Conclusion: The observed B cell dynamics provided insights into the immunological mechanisms underlying the therapeutic effects of anti-BAFF in SLE patients. Furthermore, it underscores the need for research in predicting drug responses based on immune profiling.
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