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Myo1g is required for efficient adhesion and migration of activated B lymphocytes to inguinal lymph nodes

David Cruz‐Zárate, Orestes López‐Ortega, Daniel Alberto Girón‐Pérez, Alan M. Gonzalez‐Suarez, José L. García-Cordero, Michael Schnoor, Leopoldo Santos‐Argumedo

2021Scientific Reports18 citationsDOIOpen Access PDF

Abstract

Cell migration is a dynamic process that involves adhesion molecules and the deformation of the moving cell that depends on cytoskeletal remodeling and actin-modulating proteins such as myosins. In this work, we analyzed the role of the class I Myosin-1 g (Myo1g) in migratory processes of LPS + IL-4 activated B lymphocytes in vivo and in vitro. In vivo, the absence of Myo1g reduced homing of activated B lymphocytes into the inguinal lymph node. Using microchannel chambers and morphology analysis, we found that the lack of Myo1g caused adhesion and chemotaxis defects. Additionally, deficiency in Myo1g causes flaws in adopting a migratory morphology. Our results highlight the importance of Myo1g during B cell migration.

Topics & Concepts

Cell biologyHoming (biology)MyosinCell migrationActinIn vivoCell adhesion moleculeCytoskeletonCell adhesionIn vitroChemotaxisLymphocyte homing receptorBiologyAdhesionChemistryCellGeneticsReceptorOrganic chemistryEcologyCellular Mechanics and InteractionsMuscle Physiology and DisordersCell Adhesion Molecules Research
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