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Lck Mediates Signal Transmission from CD59 to the TCR/ CD3 Pathway in Jurkat T Cells

  • Anna M. Lipp
  • , Kata Juhasz
  • , Christian Paar
  • , Christoph Ogris
  • , P. Eckerstorfer
  • , Roland Thuenauer
  • , Jan Hesse
  • , Benedikt Nimmervoll
  • , Hannes Stockinger
  • , Gerhard Schütz
  • , Ulrich Bodenhofer
  • , Zsolt Balogi
  • , Alois Sonnleitner

Research output: Contribution to journalArticlepeer-review

Abstract

The glycosylphosphatidylinositol (GPI)-anchored molecule CD59 has been implicated in the modulation of T cell responses, but the underlying molecular mechanism of CD59 influencing T cell signaling remained unclear. Here we analyzed Jurkat T cells stimulated via anti-CD3ε- or anti-CD59-coated surfaces, using time-resolved single-cell Ca2+ imaging as a read-out for stimulation. This analysis revealed a heterogeneous Ca2+ response of the cell population in a stimulus-dependent manner. Further analysis of T cell receptor (TCR)/CD3 deficient or overexpressing cells showed that CD59-mediated signaling is strongly dependent on TCR/CD3 surface expression. In protein co-patterning and fluorescence recovery after photobleaching experiments no direct physical interaction was observed between CD59 and CD3 at the plasma membrane upon anti-CD59 stimulation. However, siRNA-mediated protein knock-downs of downstream signaling molecules revealed that the Src family kinase Lck and the adaptor molecule linker of activated T cells (LAT) are essential for both signaling pathways. Furthermore, flow cytometry measurements showed that knock-down of Lck accelerates CD3 re-expression at the cell surface after anti-CD59 stimulation similar to what has been observed upon direct TCR/CD3 stimulation. Finally, physically linking Lck to CD3ζ completely abolished CD59-triggered Ca2+ signaling, while signaling was still functional upon direct TCR/CD3 stimulation. Altogether, we demonstrate that Lck mediates signal transmission from CD59 to the TCR/CD3 pathway in Jurkat T cells, and propose that CD59 may act via Lck to modulate T cell responses.
Original languageEnglish
Article numbere85934
Number of pages12
JournalPLOS One
Volume9
Issue number1
DOIs
Publication statusPublished - 15 Jan 2014

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

  1. SDG 3 - Good Health and Well-being
    SDG 3 Good Health and Well-being

Fields of science

  • 303 Health Sciences
  • 304 Medical Biotechnology
  • 305 Other Human Medicine, Health Sciences
  • 101004 Biomathematics
  • 101029 Mathematical statistics
  • 102 Computer Sciences
  • 102001 Artificial intelligence
  • 102015 Information systems
  • 102018 Artificial neural networks
  • 102022 Software development
  • 106013 Genetics
  • 106023 Molecular biology
  • 106002 Biochemistry
  • 106005 Bioinformatics
  • 106041 Structural biology
  • 301 Medical-Theoretical Sciences, Pharmacy
  • 302 Clinical Medicine

JKU Focus areas

  • Computation in Informatics and Mathematics
  • Nano-, Bio- and Polymer-Systems: From Structure to Function

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