8
Autotaxin/lysopholipase D and lysophosphatidic acid regulate murine hemostasis and thrombosis.
J Biol Chem. 2009 Mar 13; 284(11):7385-94
Xiaoping Du, University of Illinois, IL, USA. F1000 Pharmacology & Drug Discovery
18 Feb 2009 | New Finding
This interesting paper demonstrates that lysophosphatidic acid (LPA) and LPA-generating enzyme lysophospholipase D (autotaxin) inhibits mouse platelet function and plays an important inhibitory role in hemostasis and thrombosis in vivo in a transgenic mouse model. This finding is in contrast to the previous reports that LPA stimulates human platelet activation, and reveals a novel regulatory role of LPA in platelet function and atherothrombosis.
LPA is a lipid that is enriched in atherosclerosis plaques, and was previously shown to stimulate platelet activation in human platelets. Thus, it is believed that LPA may be important in the development of atherothrombosis. However, platelets from a percentage of human donors do not respond to LPA stimulation. This article reports that LPA in fact inhibits platelet function in this mouse model and that overexpression of the LPA-generating enzyme lysophospholipase D (autotaxin) in mice causes bleeding, which is recapitulated by LPA injection, indicating an important negative regulatory role of LPA in platelet function and in thrombus formation. Future studies on the difference between human platelet studies and mouse should help our understanding of the role of LPA in atherosclerosis and thrombosis.
Competing interests: None declared
Du X: "This interesting paper demonstrates that lysophosphatidic acid (LPA) and LPA-generating enzyme lysophospholipase D (autotaxin) inhibits..." Evaluation of: [Pamuklar Z et al. Autotaxin/lysopholipase D and lysophosphatidic acid regulate murine hemostasis and thrombosis. J Biol Chem. 2009 Mar 13; 284(11):7385-94; doi: 10.1074/jbc.M807820200]. Faculty of 1000, 18 Feb 2009. F1000.com/1148842#eval605927
Short form
Du X: 2009. F1000.com/1148842#eval605927
Faculty of 1000 evaluations, dissents and comments for [Pamuklar Z et al. Autotaxin/lysopholipase D and lysophosphatidic acid regulate murine hemostasis and thrombosis. J Biol Chem. 2009 Mar 13; 284(11):7385-94; doi: 10.1074/jbc.M807820200]. Faculty of 1000, 18 Feb 2009. F1000.com/1148842
Short form
Faculty of 1000: 2009. F1000.com/1148842
The lipid mediator lysophosphatidic acid (LPA) is a potent regulator of vascular cell function in vitro, but its physiologic role in the cardiovasculature is largely unexplored. To address the role of LPA in regulating platelet function and thrombosis, we investigated the effects of LPA on isolated murine platelets. Although LPA activates platelets from the majority of human donors, we found that treatment of isolated murine platelets with physiologic concentrations of LPA attenuated agonist-induced aggregation. Transgenic overexpression of autotaxin/lysophospholipase D (Enpp2), the enzyme necessary for production of the bulk of biologically active LPA in plasma, elevated circulating LPA levels and induced a bleeding diathesis and attenuation of thrombosis in mice. Intravascular administration of exogenous LPA recapitulated the prolonged bleeding time observed in Enpp2-Tg mice. Enpp2+/- mice, which have approximately 50% normal plasma LPA levels, were more prone to thrombosis. Plasma autotaxin associated with platelets during aggregation and concentrated in arterial thrombus, and activated but not resting platelets bound recombinant autotaxin/lysoPLD in an integrin-dependent manner. These results identify a novel pathway in which LPA production by autotaxin/lysoPLD regulates murine hemostasis and thrombosis and suggest that binding of autotaxin/lysoPLD to activated platelets may provide a mechanism to localize LPA production.
DOI: 10.1074/jbc.M807820200
PMID: 19139100
Sign in/get access to leave a comment.
No comments yet.