Abstract
Glycoprotein (GP) VI is the major platelet collagen receptor and a promising anti-thrombotic target. This was first demonstrated in mice using the rat monoclonal antibody JAQ1, which completely blocks the Collagen-Related Peptide (CRP)-binding site on mouse GPVI and efficiently inhibits mouse platelet adhesion, activation and aggregation on collagen. Here, we show for the first time that JAQ1 cross-reacts with human GPVI (huGPVI), but not with GPVI in other tested species, including rat, rabbit, guinea pig, swine, and dog. We further demonstrate that JAQ1 differently modulates mouse and human GPVI function. Similar to its effects on mouse GPVI (mGPVI), JAQ1 inhibits CRP-induced activation in human platelets, whereas, in stark contrast to mouse GPVI, it does not inhibit the adhesion, activation or aggregate formation of human platelets on collagen, but causes instead an increased response. This effect was also seen with platelets from newly generated human GPVI knockin mice (hGP6tg/tg). These results indicate that the binding of JAQ1 to a structurally conserved epitope in GPVI differently affects its function in human and mouse platelets.
Original language | English |
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Article number | 8610 |
Number of pages | 12 |
Journal | International journal of molecular sciences |
Volume | 23 |
Issue number | 15 |
DOIs | |
Publication status | Published - 3 Aug 2022 |
Keywords
- Animals
- Blood Platelets/metabolism
- Collagen/metabolism
- Dogs
- Epitopes/metabolism
- Guinea Pigs
- Humans
- Mice
- Platelet Activation
- Platelet Adhesiveness
- Platelet Aggregation
- Platelet Membrane Glycoproteins/metabolism
- Rabbits
- Rats
- ACTIVATION
- COLLAGEN RECEPTOR
- DEPLETION
- platelet activation
- JAQ1
- glycoprotein VI
- platelet inhibition
- MODEL
- FIBRIN
- platelet receptors
- PLATELET GLYCOPROTEIN-VI