Siponimod enriches regulatory T and B lymphocytes in secondary progressive multiple sclerosis
Qi Wu, Elizabeth A. Mills, Qin Wang, Catherine A. Dowling, Caitlyn Fisher, Britany Kirch, Steven K. Lundy, David A. Fox, Yang Mao-Draayer, the AMS04 Study Group
Qi Wu, Elizabeth A. Mills, Qin Wang, Catherine A. Dowling, Caitlyn Fisher, Britany Kirch, Steven K. Lundy, David A. Fox, Yang Mao-Draayer, the AMS04 Study Group
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Clinical Research and Public Health

Siponimod enriches regulatory T and B lymphocytes in secondary progressive multiple sclerosis

Abstract

BACKGROUND Siponimod (BAF312) is a selective sphingosine-1-phosphate receptor 1 and 5 (S1PR1, S1PR5) modulator recently approved for active secondary progressive multiple sclerosis (SPMS). The immunomodulatory effects of siponimod in SPMS have not been previously described.METHODS We conducted a multicentered, randomized, double-blind, placebo-controlled AMS04 mechanistic study with 36 SPMS participants enrolled in the EXPAND trial. Gene expression profiles were analyzed using RNA derived from whole blood with Affymetrix Human Gene ST 2.1 microarray technology. We performed flow cytometry–based assays to analyze the immune cell composition and microarray gene expression analysis on peripheral blood from siponimod-treated participants with SPMS relative to baseline and placebo during the first-year randomization phase.RESULTS Microarray analysis showed that immune-associated genes involved in T and B cell activation and receptor signaling were largely decreased by siponimod, which is consistent with the reduction in CD4+ T cells, CD8+ T cells, and B cells. Flow cytometric analysis showed that within the remaining lymphocyte subsets there was a reduction in the frequencies of CD4+ and CD8+ naive T cells and central memory cells, while T effector memory cells, antiinflammatory Th2, and T regulatory cells (Tregs) were enriched. Transitional regulatory B cells (CD24hiCD38hi) and B1 cell subsets (CD43+CD27+) were enriched, shifting the balance in favor of regulatory B cells over memory B cells. The proregulatory shift driven by siponimod treatment included a higher proliferative potential of Tregs compared with non-Tregs, and upregulated expression of PD-1 on Tregs. Additionally, a positive correlation was found between Tregs and regulatory B cells in siponimod-treated participants.CONCLUSION The shift toward an antiinflammatory and suppressive homeostatic immune system may contribute to the clinical efficacy of siponimod in SPMS.TRIAL REGISTRATION NCT02330965.

Authors

Qi Wu, Elizabeth A. Mills, Qin Wang, Catherine A. Dowling, Caitlyn Fisher, Britany Kirch, Steven K. Lundy, David A. Fox, Yang Mao-Draayer, the AMS04 Study Group

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Figure 11

Tregs that are increased in frequency after siponimod treatment exhibit increased proliferation.

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Tregs that are increased in frequency after siponimod treatment exhibit ...
(A) Representative FACS profile of CD4+ T cells from patient before and after treatment with siponimod (12 months) or placebo (10 months, end of study). (B) Cross-sectional comparison of Ki67+ percentage of FoxP3+CD4+ T cells at baseline, 6 months, and 9–12 months after treatment with placebo (0 months, n = 8; 6 months, n = 8; 9–12 months, n = 12) or siponimod (0 months, n = 13; 6 months, n = 13; 9–12 months, n = 16). (C) Increased PD-1+ frequency of CD4+ T cells in 9–12 month siponimod-treated patients (n = 10) compared with 9–12 month placebo-treated patients (n = 7). Numbers above the data symbols represent P values where the difference between placebo and siponimod is statistically significant at the same time points. Unpaired t test was used for A, 0 and 9–12 months. Mann-Whitney U test was used for A, 9–12 months; and C.