PLoS ONE (Jan 2014)

Pathogen sensing pathways in human embryonic stem cell derived-endothelial cells: role of NOD1 receptors.

  • Daniel M Reed,
  • Gabor Foldes,
  • Timothy Gatheral,
  • Koralia E Paschalaki,
  • Zsuzsanna Lendvai,
  • Zsolt Bagyura,
  • Tamas Nemeth,
  • Judit Skopal,
  • Bela Merkely,
  • Aurica G Telcian,
  • Leila Gogsadze,
  • Michael R Edwards,
  • Peter J Gough,
  • John Bertin,
  • Sebastian L Johnston,
  • Sian E Harding,
  • Jane A Mitchell

DOI
https://doi.org/10.1371/journal.pone.0091119
Journal volume & issue
Vol. 9, no. 4
p. e91119

Abstract

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Human embryonic stem cell-derived endothelial cells (hESC-EC), as well as other stem cell derived endothelial cells, have a range of applications in cardiovascular research and disease treatment. Endothelial cells sense Gram-negative bacteria via the pattern recognition receptors (PRR) Toll-like receptor (TLR)-4 and nucleotide-binding oligomerisation domain-containing protein (NOD)-1. These pathways are important in terms of sensing infection, but TLR4 is also associated with vascular inflammation and atherosclerosis. Here, we have compared TLR4 and NOD1 responses in hESC-EC with those of endothelial cells derived from other stem cells and with human umbilical vein endothelial cells (HUVEC). HUVEC, endothelial cells derived from blood progenitors (blood outgrowth endothelial cells; BOEC), and from induced pluripotent stem cells all displayed both a TLR4 and NOD1 response. However, hESC-EC had no TLR4 function, but did have functional NOD1 receptors. In vivo conditioning in nude rats did not confer TLR4 expression in hESC-EC. Despite having no TLR4 function, hESC-EC sensed Gram-negative bacteria, a response that was found to be mediated by NOD1 and the associated RIP2 signalling pathways. Thus, hESC-EC are TLR4 deficient but respond to bacteria via NOD1. This data suggests that hESC-EC may be protected from unwanted TLR4-mediated vascular inflammation, thus offering a potential therapeutic advantage.