Long-lived plasma cells are early and constantly generated in New Zealand Black/New Zealand White F1 mice and their therapeutic depletion requires a combined targeting of autoreactive plasma cells and their precursors.

Adriano Taddeo,Tobias Alexander,Bimba F Hoyer,Katrin Moser,Qingyu Cheng,Rudolf A Manz,Imtiaz M Mumtaz,Laleh Khodadadi,Andreas Radbruch,Falk Hiepe,Caroline Voigt

doi:10.1186/s13075-015-0551-3

Adriano Taddeo, Tobias Alexander + Show 9 more

Open Access

https://doi.org/10.1186/s13075-015-0551-3

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Abstract

IntroductionAutoantibodies contribute significantly to the pathogenesis of systemic lupus erythematosus (SLE). Unfortunately, the long-lived plasma cells (LLPCs) secreting such autoantibodies are refractory to conventional immunosuppressive treatments. Although generated long before the disease becomes clinically apparent, it remains rather unclear whether LLPC generation continues in the established disease. Here, we analyzed the generation of LLPCs, including autoreactive LLPCs, in SLE-prone New Zealand Black/New Zealand White F1 (NZB/W F1) mice over their lifetime, and their regeneration after depletion.MethodsBromodeoxyuridine pulse-chase experiments in mice of different ages were performed in order to analyze the generation of LLPCs during the development of SLE. LLPCs were enumerated by flow cytometry and autoreactive anti-double-stranded DNA (anti-dsDNA) plasma cells by enzyme-linked immunospot (ELISPOT). For analyzing the regeneration of LLPCs after depletion, mice were treated with bortezomib alone or in combination with cyclophosphamide and plasma cells were enumerated 12 hours, 3, 7, 11 and 15 days after the end of the bortezomib cycle.ResultsAutoreactive LLPCs are established in the spleen and bone marrow of SLE-prone mice very early in ontogeny, before week 4 and before the onset of symptoms. The generation of LLPCs then continues throughout life. LLPC counts in the spleen plateau by week 10, but continue to increase in the bone marrow and inflamed kidney. When LLPCs are depleted by the proteasome inhibitor bortezomib, their numbers regenerate within two weeks. Persistent depletion of LLPCs was achieved only by combining a cycle of bortezomib with maintenance therapy, for example cyclophosphamide, depleting the precursors of LLPCs or preventing their differentiation into LLPCs.ConclusionsIn SLE-prone NZB/W F1 mice, autoreactive LLPCs are generated throughout life. Their sustained therapeutic elimination requires both the depletion of LLPCs and the inhibition of their regeneration.

Highlights

Autoantibodies contribute significantly to the pathogenesis of systemic lupus erythematosus (SLE)
When long-lived plasma cell (LLPC) are depleted by the proteasome inhibitor bortezomib, their numbers regenerate within two weeks
In SLE-prone NZB/W F1 mice, autoreactive LLPCs are generated throughout life

Summary

Introduction

Autoantibodies contribute significantly to the pathogenesis of systemic lupus erythematosus (SLE). We have shown before that these mice develop both long-lived and short-lived autoreactive plasma cells, and that long-lived plasma cells (LLPCs) contribute significantly to the production of pathogenic autoantibodies [3] These LLPCs are able to induce nephritis when transferred into immunodeficient mice [4]. We have previously shown that a population of autoreactive LLPCs exists in the spleen and bone marrow by week 24 of life [3] Whether such population is established early in disease pathogenesis and no longer formed later, when constant generation of short-lived plasma cells (SLPCs) may become a hallmark of pathology [12], remain unclear. Interesting studies showed that B cells are able to repopulate the plasma cell-deficient bone marrow [15], it remains rather unclear whether in autoimmunity LLPCs may be replenished from autoreactive memory B cells after therapeutic depletion of these cells

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