Lymphocyte perform reverse adhesive haptotaxis mediated by integrins LFA-1

Author:

Luo Xuan1,Seveau de Noray Valentine1,Aoun Laurene1,Biarnes-Pelicot Martine1,Strale Pierre-Olivier2,Studer Vincent34,Valignat Marie-Pierre1,Theodoly Olivier1ORCID

Affiliation:

1. LAI, Aix Marseille Univ, CNRS, INSERM, Marseille, France

2. ALVEOLE, Paris, France

3. University of Bordeaux, Interdisciplinary Institute for Neuroscience, Bordeaux, France

4. CNRS UMR 5297, F-33000 Bordeaux, France

Abstract

Cell Guidance by anchored molecules, or haptotaxis, is crucial in development, immunology and cancer. Adhesive haptotaxis, or guidance by adhesion molecules, is well established for mesenchymal cells like fibroblasts, whereas its existence remains unreported for amoeboid cells that require less or no adhesion to migrate. We show here in vitro that amoeboid human T lymphocytes develop adhesive haptotaxis versus densities of integrin ligands expressed by high endothelial venules. Moreover, lymphocytes orient towards increasing adhesion with VLA-4 integrins, like all mesenchymal cells, but towards decreasing adhesion with LFA-1 integrins, which has never been observed. This counterintuitive ‘reverse haptotaxis’ cannot be explained with the existing mesenchymal mechanisms of competition between cells’ pulling edges or of lamellipodia growth activated by integrins, which favor orientation towards increasing adhesion. Mechanisms and functions of amoeboid adhesive haptotaxis remain unclear, however multidirectional integrin-mediated haptotaxis may operate around transmigration ports on endothelium, stromal cells in lymph nodes, and inflamed tissue where integrin ligands are spatially modulated.

Funder

Agence Nationale de la Recherche

ok

Region Sud

Turing center for living systems

excellence intiative of aix marseille université AMIDEX

Publisher

The Company of Biologists

Subject

Cell Biology

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