Temporalmente, el archivo digital asociado a esta publicación, no se encuentra disponible. Para más información escribir a [email protected]
Este documento se encuentra disponible en su fuente de origen, si desea acceder al texto completo, puedes hacerlo a continuación:
Autor(es)
Ibañez-Vega, Jorge; Del Valle Batalla, Felipe; Saez, Juan José; Soza, Andrea; Yuseff, Maria Isabel |
ISSN:
1664-3224 |
Idioma:
eng |
Fecha:
2019 |
Tipo:
Artículo |
Revista:
Frontiers in Immunology |
Datos de la publicación:
vol. 10 Issue: no. FEB Pages: |
DOI:
10.3389/fimmu.2019.00225 |
Descripción:
Publisher Copyright: Copyright © 2019 Ibañez-Vega, Del Valle Batalla, Saez, Soza and Yuseff. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms. |
Resumen:
Engagement of the B cell receptor (BCR) with surface-tethered antigens leads to the formation of an immune synapse (IS), where cell signaling and antigen uptake are tightly coordinated. Centrosome re-orientation to the immune synapse has emerged as a critical regulatory step to guide the local recruitment and secretion of lysosomes, which can facilitate the extraction of immobilized antigens. This process is coupled to actin remodeling at the centrosome and at the immune synapse, which is crucial to promote cell polarity. How B cells balance both pools of actin cytoskeleton to achieve a polarized phenotype during the formation of an immune synapse is not fully understood. Here, we reveal that B cells rely on proteasome activity to achieve this task. The proteasome is a multi-catalytic protease that degrades cytosolic and nuclear proteins and its dysfunction is associated with diseases, such as cancer and autoimmunity. Our results show that resting B cells contain an active proteasome pool at the centrosome, which is required for efficient actin clearance at this level. As a result of proteasome inhibition, activated B cells do not deplete actin at the centrosome and are unable to separate the centrosome from the nucleus and thus display impaired polarity. Consequently, lysosome recruitment to the immune synapse, antigen extraction and presentation are severely compromised in B cells with diminished proteasome activity. Additionally, we found that proteasome inhibition leads to impaired actin remodeling at the immune synapse, where B cells display defective spreading responses and distribution of key signaling molecules at the synaptic membrane. Overall, our results reveal a new role for the proteasome in regulating the immune synapse of B cells, where the intracellular compartmentalization of proteasome activity controls cytoskeleton remodeling between the centrosome and synapse, with functional repercussions in antigen extraction and presentation. |
Ficheros | Tamaño | Formato | Ver |
---|---|---|---|
No hay ficheros asociados a este ítem. |
El Repositorio Institucional de la Universidad San Sebastián reúne los trabajos académicos y de investigación elaborados por la comunidad universitaria. Contribuye a la visibilidad y difusión, para ser consultados a través de acceso abierto por toda la comunidad nacional e internacional.
El objetivo del Repositorio es almacenar, conservar y entregar en formato electrónico, los resultados del quehacer institucional, permitiendo mayor visibilidad y difusión por medio del acceso abierto y gratuito.