PLoS ONE (Jan 2013)

Association of the LILRA3 deletion with B-NHL and functional characterization of the immunostimulatory molecule.

  • Hui Zhi Low,
  • Sandra Reuter,
  • Michael Topperwien,
  • Nadine Dankenbrink,
  • Dietrich Peest,
  • Gamze Kabalak,
  • Renata Stripecke,
  • Reinhold E Schmidt,
  • Torsten Matthias,
  • Torsten Witte

DOI
https://doi.org/10.1371/journal.pone.0081360
Journal volume & issue
Vol. 8, no. 12
p. e81360

Abstract

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LILRA3 is the sole soluble member of the LILR family. Previous studies from our group had shown that a 6.7 kb genetic deletion of LILRA3 is associated with MS and Sjögren's syndrome. An impairment of the immune response leads to a predisposition for B-NHL, so we wanted to study whether the deletion of LILRA3 is also a risk factor for B-NHL, as well as the function of LILRA3. We discovered that the frequency of the homozygous LILRA3 deletion was significantly higher in B-NHL (6%) than in blood donors (3%) (P = 0.03). We detected binding of fluorochrome-conjugated recombinant LILRA3 to monocytes and B-cells. Incubation of PBMCs with recombinant LILRA3 induced proliferation of CD8(+) T-cells and NK cells, as determined by CFSE staining. Using a transwell system, we demonstrated that LILRA3-stimulated lymphocyte proliferation was mediated by monocytes and required both cell contact and soluble factors. Secretion of IL-6, IL-8, IL-1β and IL-10 in the cell supernatant was stimulated by LILRA3. We conclude that LILRA3 is an immunostimulatory molecule, whose deficiency is associated with higher frequency of B-NHL.