Gray platelet syndrome and defective thrombo-inflammation in Nbeal2-deficient mice
Carsten Deppermann, … , David Stegner, Bernhard Nieswandt
Carsten Deppermann, … , David Stegner, Bernhard Nieswandt
Published July 1, 2013
Citation Information: J Clin Invest. 2013;123(8):3331-3342. https://doi.org/10.1172/JCI69210.
View: Text | PDF
Research Article Hematology

Gray platelet syndrome and defective thrombo-inflammation in Nbeal2-deficient mice

Abstract

Platelets are anuclear organelle-rich cell fragments derived from bone marrow megakaryocytes (MKs) that safeguard vascular integrity. The major platelet organelles, α-granules, release proteins that participate in thrombus formation and hemostasis. Proteins stored in α-granules are also thought to play a role in inflammation and wound healing, but their functional significance in vivo is unknown. Mutations in NBEAL2 have been linked to gray platelet syndrome (GPS), a rare bleeding disorder characterized by macrothrombocytopenia, with platelets lacking α-granules. Here we show that Nbeal2-knockout mice display the characteristics of human GPS, with defective α-granule biogenesis in MKs and their absence from platelets. Nbeal2 deficiency did not affect MK differentiation and proplatelet formation in vitro or platelet life span in vivo. Nbeal2-deficient platelets displayed impaired adhesion, aggregation, and coagulant activity ex vivo that translated into defective arterial thrombus formation and protection from thrombo-inflammatory brain infarction following focal cerebral ischemia. In a model of excisional skin wound repair, Nbeal2-deficient mice exhibited impaired development of functional granulation tissue due to severely reduced differentiation of myofibroblasts in the absence of α-granule secretion. This study demonstrates that platelet α-granule constituents are critically required not only for hemostasis but also thrombosis, acute thrombo-inflammatory disease states, and tissue reconstitution after injury.

Authors

Carsten Deppermann, Deya Cherpokova, Paquita Nurden, Jan-Niklas Schulz, Ina Thielmann, Peter Kraft, Timo Vögtle, Christoph Kleinschnitz, Sebastian Dütting, Georg Krohne, Sabine A. Eming, Alan T. Nurden, Beate Eckes, Guido Stoll, David Stegner, Bernhard Nieswandt

×

Figure 1

Nbeal2–/– mice are macrothrombocytopenic and lack platelet α-granules.

Options: View larger image (or click on image) Download as PowerPoint
Nbeal2–/– mice are macrothrombocytopenic and lack platelet α-granules. ...
(A) Analysis of Nbeal2 mRNA in bone marrow (b) and thymus (t) in wild-type (+/+) and Nbeal2–/– (–/–) mice. Gapdh mRNA served as loading control. (B) Spleen to body weight ratio was analyzed in 6-week-old and 6-month-old mice. Values are mean ± SD (n = 4). (C) Peripheral platelet counts and mean platelet volume (MPV) in wild-type and Nbeal2–/– mice. Values are mean ± SD (n = 7). (D) Platelet life span as measured by injection of DyLight 488 α-GPIX. (E) Determination of MK numbers per visual field (294 × 221 μm) in H&E-stained spleen and bone marrow sections of 6-week-old and 6-month-old mice. Values are mean ± SD (n = 4). *P < 0.05; **P < 0.01; ***P < 0.001.