# B cells maintain the homeostasis of splenic marginal zone antigen-presenting cells to promote the antiviral CD8+ T-cell response

**Authors:** Xinyuan Liu, Filiz Demircik, Mariia Antipova, Emmanouil Stylianakis, Matthias Klein, David Bejarano, Abdelrahman Elwy, Anna Ebering, Michaela Blanfeld, Katlynn Carter, Lisa Johann, David C. Uhlfelder, Elisa Blickberndt, Yao Chen, Hans Christian Probst, Nadine Hövelmeyer, Tobias Bopp, Ramon Arens, Lukas Bunse, Joke M. M. den Haan, Jennifer L. Gommerman, Esther von Stebut, Björn E. Clausen, Andreas Schlitzer, Karl S. Lang, Bing Su, Ronald A. Backer, Niels A. Lemmermann, Ari Waisman

PMC · DOI: 10.1038/s41423-026-01392-0 · 2026-02-24

## TL;DR

B cells help maintain immune cells in the spleen, which in turn support CD8+ T cells to fight viruses like CMV.

## Contribution

B cells support antiviral CD8+ T-cell responses by maintaining splenic antigen-presenting cell homeostasis, not through antibody production.

## Key findings

- B-cell-deficient mice had weaker CD8+ T-cell responses and higher viral transcription.
- B cells sustain Langerin+ cDC1s via LTβ to maintain CD169+ marginal macrophages.
- VCAM1–ITGA4/ITGB1 interaction mediates communication between macrophages and cDC1s.

## Abstract

Natural killer and CD8+ T cells are critical in the elimination of blood-borne viruses such as cytomegalovirus (CMV); however, the role of B cells in this process is less clear. Here, using a murine CMV (MCMV) infection model, we demonstrated that B-cell-deficient mice mounted a weaker primary virus-specific CD8+ T-cell response than their wild-type counterparts did, which was associated with increased viral transcription. Notably, we found that the contribution of B cells to the CD8+ T-cell-mediated antiviral response was not associated with their ability to generate antibodies but with their ability to sustain Langerin+ type 1 conventional dendritic cells (cDC1s), a dendritic cell (DC) subset known for being involved in viral and bacterial clearance in the marginal zone of the spleen. Furthermore, we found that the presence of Langerin+ cDC1s is dependent on B cells expressing lymphotoxin (LTβ) to maintain CD169+ marginal metallophilic macrophages (MMMs). We further discovered, via ligand‒receptor interaction analyses, that the communication between MMMs and Langerin+ cDC1s was mediated via the VCAM1–ITGA4/ITGB1 interaction. Thus, our data reveal that B cells regulate the development of MMMs in the spleen via LTβ expression and consequently sustain Langerin+ cDC1 homeostasis for effective initiation of an antiviral CD8+ T-cell response. Overall, our study offers a new perspective on how B cells maintain the homeostasis of antigen-presenting cells in the splenic marginal zone and thus indirectly affect the virus-specific CD8+ T-cell response, which could be extended to other infectious and autoimmune diseases as well as tumors.

## Linked entities

- **Genes:** LTB (lymphotoxin beta) [NCBI Gene 4050], VCAM1 (vascular cell adhesion molecule 1) [NCBI Gene 7412], ITGA4 (integrin subunit alpha 4) [NCBI Gene 3676], ITGB1 (integrin subunit beta 1) [NCBI Gene 3688]
- **Species:** Mus musculus (taxon 10090)

## Full-text entities

- **Genes:** Siglec1 (sialic acid binding Ig-like lectin 1, sialoadhesin) [NCBI Gene 20612] {aka Cd169, Siglec-1, Sn}, Ltb (lymphotoxin B) [NCBI Gene 16994] {aka LTbeta, Tnfc, Tnfsf3, Tnlg1c, p33}, Itga4 (integrin alpha 4) [NCBI Gene 16401] {aka CD49D, Itga4B}, Itgb1 (integrin beta 1 (fibronectin receptor beta)) [NCBI Gene 16412] {aka 4633401G24Rik, CD29, Fnrb, Gm9863, gpIIa}, Vcam1 (vascular cell adhesion molecule 1) [NCBI Gene 22329] {aka CD106, Vcam-1}, Cd207 (CD207 antigen) [NCBI Gene 246278]
- **Diseases:** tumors (MESH:D009369), infection (MESH:D007239), CMV (MESH:D003586), autoimmune diseases (MESH:D001327), infectious (MESH:D003141)
- **Species:** Mus musculus (house mouse, species) [taxon 10090]

## Figures

6 figures with captions in the complete paper: https://tomesphere.com/paper/PMC13035995/full.md

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Source: https://tomesphere.com/paper/PMC13035995