# CD72 downregulation on DN2 B cells is associated with disease activity and resistance to rituximab in systemic lupus erythematosus

**Authors:** Kittikorn Wangriatisak, Wenqi Huang, Giorgio Sechi, Vilija Oke, Karine Chemin, Caroline Grönwall, Iva Gunnarsson, Vivianne Malmström, Francesca Faustini

PMC · DOI: 10.1093/rheumatology/keag097 · Rheumatology (Oxford, England) · 2026-02-18

## TL;DR

A study finds that B cells with low CD72 levels in lupus patients are linked to disease activity and resistance to treatment.

## Contribution

The study identifies CD72 downregulation on DN2 B cells as a novel biomarker for lupus disease activity and RTX resistance.

## Key findings

- CD72-negative DN2 B cells are elevated in active lupus patients and correlate with anti-dsDNA positivity and complement consumption.
- CD72-negative B cells show increased BCR signaling and are relatively resistant to rituximab treatment.
- These cells may contribute to lupus relapse due to impaired checkpoint regulation.

## Abstract

In SLE, expanded B cell subtypes like double-negative 2 (DN2) may harbour autoreactivity, which may be linked to impaired checkpoint regulation. We investigated checkpoint molecule CD72 on B cells, its clinical associations, and dynamic changes upon rituximab (RTX) treatment.

Thirty SLE patients (26 with active disease) were studied. Seven received RTX treatment with sampling at baseline, 3 months and 6 months. B cell phenotypes were analysed using spectral flow cytometry, and clinical associations were evaluated. B cell receptor (BCR) signalling was studied through downstream phosphorylation in vitro.

Patients with active SLE showed increased frequencies of CD72-negative B cells in switched memory (SWM), activated naïve (aNAV), DN2 and plasmablast (PB) subsets compared with healthy controls (HCs). CD72-negative DN2 cells (CD27-IgD-CD21-CD11c+) were elevated in LN patients. These cells expressed higher CD95 and lower CD20 compared with HCs and canonical SLE DN2. Upon BCR stimulation, lupus CD72-negative SWM and DN2 B cells displayed increased pSYK phosphorylation compared with their CD72-positive counterparts and the overall cell population. CD72-negative DN2 frequencies associated positively with SLEDAI-2K and inversely with C3 levels and were increased in anti-dsDNA-positive patients. After RTX treatment, the remaining DN2 cells were primarily CD72-negative at 3 months.

The DN2 B cell subset have been associated with autoimmunity. We showed that DN2 B cells in SLE have reduced CD72 expression, which is associated with anti-dsDNA positivity, complement consumption, and enhanced BCR downstream signalling. The relative resistance of CD72-negative B cells to RTX indicates that an impaired checkpoint programme in lupus B cells may potentially contribute to disease relapse. These findings require validation in larger cohorts.

Graphical Abstract

## Linked entities

- **Genes:** CD72 (CD72 molecule) [NCBI Gene 971], CD27 (CD27 molecule) [NCBI Gene 939], Igd (immunoglobulin delta heavy chain constant region) [NCBI Gene 641523], CR2 (complement C3d receptor 2) [NCBI Gene 1380], ITGAX (integrin subunit alpha X) [NCBI Gene 3687], FAS (Fas cell surface death receptor) [NCBI Gene 355], MS4A1 (membrane spanning 4-domains A1) [NCBI Gene 931], SYK (spleen associated tyrosine kinase) [NCBI Gene 6850]
- **Proteins:** BCR (BCR activator of RhoGEF and GTPase)
- **Diseases:** systemic lupus erythematosus (MONDO:0007915), lupus nephritis (MONDO:0005556)

## Full-text entities

- **Genes:** CD27 (CD27 molecule) [NCBI Gene 939] {aka S152, S152. LPFS2, T14, TNFRSF7, Tp55}, CR2 (complement C3d receptor 2) [NCBI Gene 1380] {aka C3DR, CD21, CR, CVID7, SLEB9}, ITGAX (integrin subunit alpha X) [NCBI Gene 3687] {aka CD11C, SLEB6}, FAS (Fas cell surface death receptor) [NCBI Gene 355] {aka ALPS1A, APO-1, APT1, CD95, FAS1, FASTM}, CD72 (CD72 molecule) [NCBI Gene 971] {aka CD72b, LYB2}, KRT20 (keratin 20) [NCBI Gene 54474] {aka CD20, CK-20, CK20, K20, KRT21}
- **Diseases:** SLE (MESH:D008180), LN (MESH:D008181)
- **Chemicals:** RTX (MESH:D000069283)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Full text

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## Figures

2 figures with captions in the complete paper: https://tomesphere.com/paper/PMC13017721/full.md

## References

20 references — full list in the complete paper: https://tomesphere.com/paper/PMC13017721/full.md

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Source: https://tomesphere.com/paper/PMC13017721