B cell depletion in immune thrombocytopenia reveals splenic long-lived plasma cells
Matthieu Mahévas, Pauline Patin, François Huetz, Marc Descatoire, Nicolas Cagnard, Christine Bole-Feysot, Simon Le Gallou, Mehdi Khellaf, Olivier Fain, David Boutboul, Lionel Galicier, Mikael Ebbo, Olivier Lambotte, Mohamed Hamidou, Philippe Bierling, Bertrand Godeau, Marc Michel, Jean-Claude Weill, Claude-Agnès Reynaud
Matthieu Mahévas, Pauline Patin, François Huetz, Marc Descatoire, Nicolas Cagnard, Christine Bole-Feysot, Simon Le Gallou, Mehdi Khellaf, Olivier Fain, David Boutboul, Lionel Galicier, Mikael Ebbo, Olivier Lambotte, Mohamed Hamidou, Philippe Bierling, Bertrand Godeau, Marc Michel, Jean-Claude Weill, Claude-Agnès Reynaud
View: Text | PDF
Research Article Autoimmunity

B cell depletion in immune thrombocytopenia reveals splenic long-lived plasma cells

Abstract

Primary immune thrombocytopenia (ITP) is a disorder caused by autoantibody-mediated platelet destruction and decreased platelet production. Rituximab, a B cell–depleting agent, has become the first-line treatment for ITP; however, patients with refractory disease usually require splenectomy. We identified antibody-secreting cells as the major splenic B cell population that is resistant to rituximab. The phenotype, antibody specificity, and gene expression profile of these cells were characterized and compared to those of antibody-secreting cells from untreated ITP spleens and from healthy tissues. Antiplatelet-specific plasma cells (PC) were detected in the spleens of patients with ITP up to 6 months after rituximab treatment, and the PC population displayed a long-lived program similar to the one of bone marrow PC, thus explaining for most of these patients the absence of response to rituximab and the response to splenectomy. When analyzed by multiplex PCR at the single-cell level, normal splenic PC showed a markedly different gene expression profile, with an intermediate signature, including genes characteristic of both long-lived PC and proliferating plasmablasts. Surprisingly, long-lived PC were not detected in untreated ITP spleens. These results suggest that the milieu generated by B cell depletion promotes the differentiation and settlement of long-lived PC in the spleen.

Authors

Matthieu Mahévas, Pauline Patin, François Huetz, Marc Descatoire, Nicolas Cagnard, Christine Bole-Feysot, Simon Le Gallou, Mehdi Khellaf, Olivier Fain, David Boutboul, Lionel Galicier, Mikael Ebbo, Olivier Lambotte, Mohamed Hamidou, Philippe Bierling, Bertrand Godeau, Marc Michel, Jean-Claude Weill, Claude-Agnès Reynaud

×

Figure 6

ASC in ITP display a prolonged in vitro survival within a specific cytokinic and cellular microenvironment.

Options: View larger image (or click on image) Download as PowerPoint
ASC in ITP display a prolonged in vitro survival within a specific cytok...
(A) ASC survival after 5-day culture. Survival was estimated by the fraction of input ASC detectable after 5-day culture of 5 × 105 spleen cells in triplicate, estimated by an anti-Ig ELISPOT (mean survival, RTX: 26.4% ± 3.7%; ITP: 32% ± 9.5%; HD: 9.3% ± 1.6%). (B) BAFF concentration in spleen supernatants after 5-day culture. BAFF concentration was estimated by ELISA in culture medium of 105 spleen cells cultured in triplicates for 5 days (mean BAFF secretion, RTX: 33.6 ± 6.2 pg/ml; ITP: 7.2 ± 1.2 pg/ml; HD: 20.2 ± 1 pg/ml). (C) CCL2 concentration in spleen supernatants after 5-day culture. CCL2 concentration was estimated as part of a multiplex 27-cytokine assay in spleen supernatants of 105 cells cultured in triplicate for 5 days (mean CCL2 secretion, RTX: 11,410 ± 228 pg/ml; ITP: 11,410 ± 1,236 pg/ml; HD: 3,233 ± 1,927 pg/ml). (D) Number of basophils in ITP and rituximab spleens. Spleen basophils were estimated by flow cytometry as numbers of HLA-DRCD123+FcεRIhi cells per 105 cells (mean basophil numbers, RTX: 1,162 ± 79.8; ITP: 591± 178.4; HD: 201 ± 64.5). (E) ASC survival from HD spleens after culture with or without BAFF (100 ng/ml). Survival was estimated as in A. The values obtained with or without BAFF for each sample are connected by a straight line (median fold increased survival with BAFF: 8.3 [3.2–23]). Significant differences estimated by Mann-Whitney and paired t test (**P < 0.01, *P < 0.05). Symbols indicate individual samples; horizontal bars represent mean values (± SEM).