4.5 Article

Differential nanoscale organisation of LFA-1 modulates T-cell migration

Journal

JOURNAL OF CELL SCIENCE
Volume 133, Issue 5, Pages -

Publisher

COMPANY BIOLOGISTS LTD
DOI: 10.1242/jcs.232991

Keywords

Integrins; LFA-1; T-cell migration; SMLM; dSTORM

Categories

Funding

  1. European Research Council [337187]
  2. Arthritis Research UK Programme [20525]
  3. King's College London Bioscience Institute
  4. Guy's and St Thomas' Charity Prize PhD Programme in Biomedical and Translational Science
  5. European Research Council (ERC) [337187] Funding Source: European Research Council (ERC)

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Effector T-cells rely on integrins to drive adhesion and migration to facilitate their immune function. The heterodimeric transmembrane integrin LFA-1 (alpha L beta 2 integrin) regulates adhesion and migration of effector T-cells through linkage of the extracellular matrix with the intracellular actin treadmill machinery. Here, we quantified the velocity and direction of F-actin flow in migrating T-cells alongside single-molecule localisation of transmembrane and intracellular LFA-1. Results showed that actin retrograde flow positively correlated and immobile actin negatively correlated with T-cell velocity. Plasma membrane-localised LFA-1 forms unique nano-clustering patterns in the leading edge, compared to the mid-focal zone, of migrating T-cells. Deleting the cytosolic phosphatase PTPN22, loss-of-function mutations of which have been linked to autoimmune disease, increased T-cell velocity, and leading-edge co-clustering of pY397 FAK, pY416 Src family kinases and LFA-1. These data suggest that differential nanoclustering patterns of LFA-1 in migrating T-cells may instruct intracellular signalling. Our data presents a paradigm where T-cells modulate the nanoscale organisation of adhesion and signalling molecules to fine tune their migration speed, with implications for the regulation of immune and inflammatory responses. This article has an associated First Person interview with the first author of the paper.

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