Identification of Tensin-3 as a MALT1 substrate that controls B cell adhesion and lymphoma dissemination

Author:

Juilland Mélanie1ORCID,Alouche Nagham1,Ubezzi Ivana1,Gonzalez Montserrat1,Rashid Harun-Or1ORCID,Scarpellino Leonardo1,Erdmann Tabea2,Grau Michael2ORCID,Lenz Georg2,Luther Sanjiv A.1ORCID,Thome Margot1ORCID

Affiliation:

1. Department of Immunobiology, University of Lausanne, Epalinges CH-1066, Switzerland

2. Department of Medicine A for Hematology, Oncology and Pneumology, University Hospital Münster, Münster D-48149, Germany

Abstract

The protease MALT1 promotes lymphocyte activation and lymphomagenesis by cleaving a limited set of cellular substrates, most of which control gene expression. Here, we identified the integrin-binding scaffold protein Tensin-3 as a MALT1 substrate in activated human B cells. Activated B cells lacking Tensin-3 showed decreased integrin-dependent adhesion but exhibited comparable NF-κB1 and Jun N-terminal kinase transcriptional responses. Cells expressing a noncleavable form of Tensin-3, on the other hand, showed increased adhesion. To test the role of Tensin-3 cleavage in vivo, mice expressing a noncleavable version of Tensin-3 were generated, which showed a partial reduction in the T cell–dependent B cell response. Interestingly, human diffuse large B cell lymphomas and mantle cell lymphomas with constitutive MALT1 activity showed strong constitutive Tensin-3 cleavage and a decrease in uncleaved Tensin-3 levels. Moreover, silencing of Tensin-3 expression in MALT1-driven lymphoma promoted dissemination of xenografted lymphoma cells to the bone marrow and spleen. Thus, MALT1-dependent Tensin-3 cleavage reveals a unique aspect of the function of MALT1, which negatively regulates integrin-dependent B cell adhesion and facilitates metastatic spread of B cell lymphomas.

Funder

Swiss National Science Foundation

Swiss Cancer Research Foundation

Emma Muschamp foundation

Deutsche Krebshilfe

Publisher

Proceedings of the National Academy of Sciences

Subject

Multidisciplinary

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