Publications by authors named "D Touchard"

Article Synopsis
  • Immune cells can move through various environments by adapting their adhesion properties using specialized proteins called integrins, which interact with different ligands and are regulated by various signals.
  • A new method was developed that uses micro-sized beads and fluid flow to study the adhesion of live T lymphocytes without disturbing their movement, revealing how certain integrins (VLA-4 and LFA-1) function differently at the front and back of the cells.
  • The study found intricate signaling relationships between integrins, highlighting that cell polarization boosts adhesion at specific sites and identifying the roles of certain proteins (Sharpin and Myosin) in regulating this adhesion process during immune cell migration.
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Contact with Leishmania leads to a decreases in mononuclear phagocyte adherence to connective tissue. In this work, we studied the early stages of bond formation between VLA4 and fibronectin, measured the kinetics of membrane alignment and the monocyte cytoplasm spreading area over a fibronectin-coated surface, and studied the expression of high affinity integrin epitope in uninfected and Leishmania-infected human monocytes. Our results show that the initial VLA4-mediated interaction of Leishmania-infected monocyte with a fibronectin-coated surface is preserved, however, the later stage, leukocyte spreading over the substrate is abrogated in Leishmania-infected cells.

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Blood leukocytes have a remarkable capacity to bind to and stop on specific blood vessel areas. Many studies have disclosed a key role of integrin structural changes following the interaction of rolling leukocytes with surface-bound chemoattractants. However, the functional significance of structural data and mechanisms of cell arrest are incompletely understood.

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Cells continually probe their environment to adapt their behaviour. A current challenge is to determine how they analyse nearby surfaces and how they process information to take decisions. We addressed this problem by monitoring human T lymphocyte attachment to surfaces coated with activating anti-CD3 or control anti-HLA antibodies.

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A critical step of the adaptive response is the detection of foreign peptides on antigen presenting cells by T lymphocytes. It is a major challenge for a T lymphocyte to detect the presence of a few tens of cognate ligands or less on the membrane of a cell exposing millions of protein molecules. Detection is followed by the cell decision to undergo full or partial activation or even to start an inhibitory program.

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