PLoS ONE (Jan 2014)

Raised soluble P-selectin moderately accelerates atherosclerotic plaque progression.

  • Kevin J Woollard,
  • Natalie G Lumsden,
  • Karen L Andrews,
  • Andrea Aprico,
  • Emma Harris,
  • Jennifer C Irvine,
  • Ann-maree Jefferis,
  • Lu Fang,
  • Peter Kanellakis,
  • Alex Bobik,
  • Jaye P F Chin-Dusting

DOI
https://doi.org/10.1371/journal.pone.0097422
Journal volume & issue
Vol. 9, no. 5
p. e97422

Abstract

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Soluble P-selectin (sP-selectin), a biomarker of inflammatory related pathologies including cardiovascular and peripheral vascular diseases, also has pro-atherosclerotic effects including the ability to increase leukocyte recruitment and modulate thrombotic responses in vivo. The current study explores its role in progressing atherosclerotic plaque disease. Apoe-/- mice placed on a high fat diet (HFD) were given daily injections of recombinant dimeric murine P-selectin (22.5 µg/kg/day) for 8 or 16 weeks. Saline or sE-selectin injections were used as negative controls. In order to assess the role of sP-selectin on atherothrombosis an experimental plaque remodelling murine model, with sm22α-hDTR Apoe-/- mice on a HFD in conjunction with delivery of diphtheria toxin to induce targeted vascular smooth muscle apoptosis, was used. These mice were similarly given daily injections of sP-selectin for 8 or 16 weeks. While plaque mass and aortic lipid content did not change with sP-selectin treatment in Apoe-/- or SM22α-hDTR Apoe-/- mice on HFD, increased plasma MCP-1 and a higher plaque CD45 content in Apoe-/- HFD mice was observed. As well, a significant shift towards a more unstable plaque phenotype in the SM22α-hDTR Apoe-/- HFD mice, with increased macrophage accumulation and lower collagen content, leading to a lower plaque stability index, was observed. These results demonstrate that chronically raised sP-selectin favours progression of an unstable atherosclerotic plaque phenotype.