T cell migration requires ion and water influx to regulate actin polymerization

Author:

de Boer Leonard L.ORCID,Vanes Lesley,Melgrati Serena,Biggs O’May Joshua,Hayward Darryl,Driscoll Paul C.ORCID,Day JasonORCID,Griffiths Alexander,Magueta Renata,Morrell AlexanderORCID,MacRae James I.ORCID,Köchl Robert,Tybulewicz Victor L. J.ORCID

Abstract

AbstractMigration of T cells is essential for their ability to mount immune responses. Chemokine-induced T cell migration requires WNK1, a kinase that regulates ion influx into the cell. However, it is not known why ion entry is necessary for T cell movement. Here we show that signaling from the chemokine receptor CCR7 leads to activation of WNK1 and its downstream pathway at the leading edge of migrating CD4+ T cells, resulting in ion influx and water entry by osmosis. We propose that WNK1-induced water entry is required to swell the membrane at the leading edge, generating space into which actin filaments can polymerize, thereby facilitating forward movement of the cell. Given the broad expression of WNK1 pathway proteins, our study suggests that ion and water influx are likely to be essential for migration in many cell types, including leukocytes and metastatic tumor cells.

Funder

Francis Crick Institute

Cancer Research UK

RCUK | Medical Research Council

Wellcome Trust

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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