Megakaryocytes endocytose and subsequently modify human factor V in vivo to form the entire pool of a unique platelet-derived cofactor

Gould, Weston R.; Simioni, Paolo; Silveira, Jay R.; Tormene, Daniela; Kalafatis, Michael; Tracy, Paula B.

doi:10.1111/j.1538-7836.2005.01157.x

Cited by 63 publications

(78 citation statements)

References 34 publications

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“…Platelet factor V is more active in supporting clotting than is plasma factor V, and in particular, platelet factor V is activated by factor Xa at an accelerated rate relative to plasma factor V (9). Platelet factor V is structurally modified compared to the plasma protein, which may help explain its enhanced activity (8,10). We propose that an additional factor enhancing the procoagulant function of platelet factor V is the concomitant secretion of polyP upon platelet activation, and that polyP serves as a cofactor to enhance the rate of factor V activation by both thrombin and factor Xa.…”

Section: Resultsmentioning

confidence: 99%

See 1 more Smart Citation

Polyphosphate modulates blood coagulation and fibrinolysis

Smith

Mutch

Baskar

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

495

623

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Inorganic polyphosphate is an abundant component of acidocalcisomes of bacteria and unicellular eukaryotes. Human platelet dense granules strongly resemble acidocalcisomes, and we recently showed that they contain substantial amounts of polyphosphate, which is secreted upon platelet activation. We now report that polyphosphate is a potent hemostatic regulator, accelerating blood clotting by activating the contact pathway and promoting the activation of factor V, which in turn results in abrogation of the function of the natural anticoagulant protein, tissue factor pathway inhibitor. Polyphosphate was also found to delay clot lysis by enhancing a natural antifibrinolytic agent, thrombin-activatable fibrinolysis inhibitor. Polyphosphate is unstable in blood or plasma, owing to the presence of phosphatases. We propose that polyphosphate released from platelets or microorganisms initially promotes clot formation and stability; subsequent degradation of polyphosphate by blood phosphatases fosters inhibition of clotting and activation of fibrinolysis during wound healing.factor V ͉ platelets ͉ tissue factor pathway inhibitor ͉ acidocalcisomes ͉ dense granules P olyphosphate (polyP) is widely distributed in biology, being found in bacteria, fungi, plants, and animals (1). The biologic functions of polyP have been studied most extensively in prokaryotes and unicellular eukaryotes, in which high levels of polyP accumulate in acidic organelles known as acidocalcisomes. PolyP in these organisms can reach chain lengths of several hundred phosphate units. In unicellular organisms, polyP has been shown to play essential roles in stress responses and virulence (1, 2), although its function in higher eukaryotes, including man, has not been extensively investigated. Recently, we reported that dense granules of human platelets strongly resemble acidocalcisomes and contain millimolar levels of polyP (with chain lengths of Ϸ70-75 phosphate units), making acidocalcisomes the only known class of organelle conserved during evolution from bacteria to humans (3). Human platelets each have three to eight dense granules (also called ␦ granules), a type of secretory granule that contains serotonin, ADP, ATP, and PP i in addition to polyP. Patients with dense granule defects exhibit bleeding diatheses, underscoring the role of these secretory granules in hemostasis (4). Platelets contain Ϸ0.74 nmol polyP per 10 8 platelets, which is secreted after stimulation by platelet agonists such as thrombin (3). Therefore, released polyP could readily attain a concentration of 3 M in whole blood, and this could be far higher in platelet-rich thrombi. (Concentrations of polyP are expressed in this paper as phosphate monomer.)The importance of platelets in hemostasis suggested to us that polyP may play an important role in the blood clotting system. In this study, we found that polyP of the size released from activated platelets has a strongly net procoagulant effect, which is exerted at several levels in the clotting͞fibrinolysis system: PolyP activate...

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Section: Resultsmentioning

confidence: 99%

“…Platelet alpha granules contain factor V, which is secreted upon platelet activation (8). Platelet factor V is more active in supporting clotting than is plasma factor V, and in particular, platelet factor V is activated by factor Xa at an accelerated rate relative to plasma factor V (9).…”

Section: Resultsmentioning

confidence: 99%

Polyphosphate modulates blood coagulation and fibrinolysis

Smith

Mutch

Baskar

et al. 2006

Proc. Natl. Acad. Sci. U.S.A.

495

623

View full text Add to dashboard Cite

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“…The platelet FV pool has been shown to originate from endocytosis of plasma FV in humans 18,32 ; although in mice, platelet FV is derived exclusively from biosynthesis within the megakaryocytes. 33,34 To address the question of whether LMAN1 and MCFD2 mutations exert differential effects between these 2 pools, we measured platelet FV antigen levels in 4 patients with LMAN1 mutations and 3 patients with MCFD2 mutations, as well as 15 healthy controls.…”

Section: Correlation Between Platelet and Plasma Fvmentioning

confidence: 99%

Genotype-phenotype correlation in combined deficiency of factor V and factor VIII

Zhang

Spreafico

Zheng

et al. 2008

Blood

111

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“…In humans, 80% of FV is found in plasma, and the remainder is stored in platelets, complexed to multimerin 1 (MMRN1), after FV is endocytosed from plasma [2][3][4]. Acquired FV inhibitors, although rare, can cause serious bleeding [5][6][7][8][9].…”

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confidence: 99%