Differing Requirements for MALT1 Function in Peripheral B Cell Survival and Differentiation

Overview

Journal J Immunol

Specialty Allergy & Immunology

Date 2016 Dec 30

PMID 28031341

Citations 4

Authors

Peishan Lee

Zilu Zhu

Janna Hachmann

Takuya Nojima

Daisuke Kitamura

Guy Salvesen

Robert C Rickert

Affiliations

Soon will be listed here.

Abstract

During a T cell-dependent immune response, formation of the germinal center (GC) is essential for the generation of high-affinity plasma cells and memory B cells. The canonical NF-κB pathway has been implicated in the initiation of GC reaction, and defects in this pathway have been linked to immune deficiencies. The paracaspase MALT1 plays an important role in regulating NF-κB activation upon triggering of Ag receptors. Although previous studies have reported that MALT1 deficiency abrogates the GC response, the relative contribution of B cells and T cells to the defective phenotype remains unclear. We used chimeric mouse models to demonstrate that MALT1 function is required in B cells for GC formation. This role is restricted to BCR signaling where MALT1 is critical for B cell proliferation and survival. Moreover, the proapoptotic signal transmitted in the absence of MALT1 is dominant to the prosurvival effects of T cell-derived stimuli. In addition to GC B cell differentiation, MALT1 is required for plasma cell differentiation, but not mitogenic responses. Lastly, we show that ectopic expression of Bcl-2 can partially rescue the GC phenotype in MALT1-deficient animals by prolonging the lifespan of BCR-activated B cells, but plasma cell differentiation and Ab production remain defective. Thus, our data uncover previously unappreciated aspects of MALT1 function in B cells and highlight its importance in humoral immunity.

Citing Articles

Progressive B cell depletion in human MALT1 deficiency.

Sonoda M, Ishimura M, Eguchi K, Yada Y, Lenhartova N, Shiraishi A Clin Exp Immunol. 2021; 206(3):237-247.

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A MALT1 inhibitor suppresses human myeloid DC, effector T-cell and B-cell responses and retains Th1/regulatory T-cell homeostasis.

Dumont C, Sivars U, Andreasson T, Odqvist L, Mattsson J, DeMicco A PLoS One. 2020; 15(9):e0222548.

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E3 Ubiquitin Ligase Fbw7 Regulates the Survival of Mature B Cells.

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