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. 2025 Aug 4;224(8):e202407181.
doi: 10.1083/jcb.202407181. Epub 2025 Jul 21.

B cell mechanotransduction via ATAT1 coordinates actin and lysosomal dynamics at the immune synapse

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B cell mechanotransduction via ATAT1 coordinates actin and lysosomal dynamics at the immune synapse

Pablo Aceitón et al. J Cell Biol. .

Abstract

B cells extract immobilized antigens via immune synapse formation, a process influenced by the physical properties of the antigen-presenting surface. However, the mechanisms linking mechanotransduction to antigen extraction and processing remain poorly understood. Here, we show that B cells activated on stiff substrates initiate mechanotransduction responses that drive the translocation of the microtubule acetylase ATAT1 from the nucleus to the cytoplasm, leading to increased α-tubulin acetylation. This modification releases GEF-H1 at the immune synapse, where it promotes the formation of actin foci essential for antigen extraction. Acetylated microtubules also enable B cells to stabilize and position lysosomes at the synapse center, thereby coupling actin-dependent extraction to antigen processing and presentation. Accordingly, ATAT1-silenced B cells fail to concentrate actin foci and lysosomes at the synaptic interface, resulting in impaired antigen extraction and presentation to T cells. Overall, these findings underscore how BCR-dependent mechanotransduction induces microtubule modifications to orchestrate lysosome positioning and actin remodeling at the immune synapse.

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