4.7 Article

Siglec-9 is a novel leukocyte ligand for vascular adhesion protein-1 and can be used in PET imaging of inflammation and cancer

Journal

BLOOD
Volume 118, Issue 13, Pages 3725-3733

Publisher

AMER SOC HEMATOLOGY
DOI: 10.1182/blood-2010-09-311076

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Funding

  1. Finnish Academy
  2. Turku University Hospital
  3. Finnish Cancer Foundation
  4. Sigrid Juselius Foundation
  5. Arvo and Inkeri Suominen Foundation
  6. National Graduate Schools in Informational and Structural Biology
  7. National Graduate Schools in Drug Discovery
  8. National Graduate Schools in Nanoscience
  9. Research Institute of the Abo Akademi Foundation
  10. Tor Foundation
  11. Joe Foundation
  12. Pentti Borg's Foundation
  13. Wellcome Trust [WT081882]
  14. Medicinska Understodsforeningen Liv och Halsa

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Leukocyte migration to sites of inflammation is regulated by several endothelial adhesion molecules. Vascular adhesion protein-1 (VAP-1) is unique among the homing-associated molecules as it is both an enzyme that oxidizes primary amines and an adhesin. Although granulocytes can bind to endothelium via a VAP-1-dependent manner, the counter-receptor(s) on this leukocyte population is(are) not known. Here we used a phage display approach and identified Siglec-9 as a candidate ligand on granulocytes. The binding between Siglec-9 and VAP-1 was confirmed by in vitro and ex vivo adhesion assays. The interaction sites between VAP-1 and Siglec-9 were identified by molecular modeling and confirmed by further binding assays with mutated proteins. Although the binding takes place in the enzymatic groove of VAP-1, it is only partially dependent on the enzymatic activity of VAP-1. In positron emission tomography, the (68)Gallium-labeled peptide of Siglec-9 specifically detected VAP-1 in vasculature at sites of inflammation and cancer. Thus, the peptide binding to the enzymatic groove of VAP-1 can be used for imaging conditions, such as inflammation and cancer. (Blood. 2011; 118(13):3725-3733)

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