Platelet ITAM signaling is critical for vascular integrity in inflammation
Yacine Boulaftali, … , Mark L. Kahn, Wolfgang Bergmeier
Yacine Boulaftali, … , Mark L. Kahn, Wolfgang Bergmeier
Published January 25, 2013
Citation Information: J Clin Invest. 2013;123(2):908-916. https://doi.org/10.1172/JCI65154.
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Research Article Hematology

Platelet ITAM signaling is critical for vascular integrity in inflammation

Abstract

Platelets play a critical role in maintaining vascular integrity during inflammation, but little is known about the underlying molecular mechanisms. Here we report that platelet immunoreceptor tyrosine activation motif (ITAM) signaling, but not GPCR signaling, is critical for the prevention of inflammation-induced hemorrhage. To generate mice with partial or complete defects in these signaling pathways, we developed a protocol for adoptive transfer of genetically and/or chemically inhibited platelets into thrombocytopenic (TP) mice. Unexpectedly, platelets with impaired GPCR signaling, a crucial component of platelet plug formation and hemostasis, were indistinguishable from WT platelets in their ability to prevent hemorrhage at sites of inflammation. In contrast, inhibition of GPVI or genetic deletion of Clec2, the only ITAM receptors expressed on mouse platelets, significantly reduced the ability of platelets to prevent inflammation-induced hemorrhage. Moreover, transfusion of platelets without ITAM receptor function or platelets lacking the adapter protein SLP-76 into TP mice had no significant effect on vascular integrity during inflammation. These results indicate that the control of vascular integrity is a major function of immune-type receptors in platelets, highlighting a potential clinical complication of novel antithrombotic agents directed toward the ITAM signaling pathway.

Authors

Yacine Boulaftali, Paul R. Hess, Todd M. Getz, Agnieszka Cholka, Moritz Stolla, Nigel Mackman, A. Phillip Owens III, Jerry Ware, Mark L. Kahn, Wolfgang Bergmeier

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Figure 4

Platelet GPCR signaling is not required for the maintenance of vascular integrity in inflammation.

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Platelet GPCR signaling is not required for the maintenance of vascular ...
(A and B) rpA reaction in skin of TP hIL-4Rα/GPIbα–Tg mice reconstituted or not (–) with the indicated platelet preparations (8 × 108 platelets/mouse; n = 15–20 spots per group). Clop, clopidogrel; ASA, aspirin. (A) Hb levels in skin lesions 4 hours after rpA challenge. Intradermal injection of PBS (without rpA) is also shown. (B) Representative images of rpA reaction sites (indicated by dashed outlines and arrows). (C and D) LPS-induced inflammation in lungs of TP hIL-4Rα/GPIbα–Tg mice reconstituted or not with the indicated platelet preparations (8 × 108 platelets/mouse; n = 5 per group). (C) Hb levels in BAL 6 hours after LPS challenge. Intradermal injection of PBS (without LPS) is also shown. (D) Representative images of BAL. ***P < 0.001 versus no platelet reconstitution.