Immobilized fibrinogen activates human platelets through glycoprotein VI

Mangin, P; Onselaer, Marie-Blanche; Receveur, Nicolas; Lay, Nicolas Le; Hardy, Alexander T.; Wilson, Clare; Sánchez, Ximena; Loyau, Stéphane; Dupuis, Arnaud; Babar, Amir K.; Miller, Jeanette L.C.; Philippou, Helen; Hughes, Craig E.; Herr, Andrew B.; Ariëns, Robert A. S.; Mezzano, Diego; Jandrot‐Perrus, Martine; Gachet, Christian; Watson, Steve P.

doi:10.3324/haematol.2017.182972

Cited by 100 publications

(97 citation statements)

References 52 publications

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“…In sharp contrast, it has been shown that this complex plays a key role in thrombus growth, for example, in platelet‐platelet interactions, by mediating the recruitment of circulating platelets to von Willebrand factor (VWF) exposed at the surface of activated platelets within the thrombus . Moreover, we recently reported that platelet aggregation under flow also involves GPVI, whereas this receptor does not participate in platelet‐platelet interactions under the low shear conditions found in LTA . In addition, the part played by soluble agonists such as thrombin, ADP, or TxA 2 might be overestimated in suspension assays like LTA where they are not washed away by the flow.…”

Section: Platelet Function Testingmentioning

confidence: 95%

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Platelet preparation for function testing in the laboratory and clinic: Historical and practical aspects

Hechler

Dupuis

Mangin

et al. 2019

Research and Practice in Thrombosis and Haemostasis

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Laboratory tests of platelet function are instrumental in studying platelet physiology and inherited or acquired platelet abnormalities. Light transmission aggregometry, developed in the early 1960s, is still considered the gold standard for the identification and diagnosis of platelet function disorders. Since then, novel techniques have been developed, including flow‐based assays and flow cytometry. In this tutorial, we describe the basic methodologies for the preparation of citrated platelet‐rich plasma and washed platelet suspensions and discuss their respective advantages and limitations as well as important factors to consider to perform high‐quality tests of platelet function. In addition, the methodologies of the main platelet function tests (light transmission aggregation, flow‐based assays, and flow cytometric assays) are described, and their respective strengths and limitations are discussed to assess various aspects of platelet biology.

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Section: Platelet Function Testingmentioning

confidence: 95%

“…Washed platelet suspensions are thus ideal for investigations using LTA, flow cytometry, electron microscopy, western blotting of platelet lysates, or radioligand binding, to mention only a few applications …”

Section: Applicationsmentioning

confidence: 99%

Platelet preparation for function testing in the laboratory and clinic: Historical and practical aspects

Hechler

Dupuis

Mangin

et al. 2019

Research and Practice in Thrombosis and Haemostasis

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“…In one study, the GPVI‐fibrin interaction occurred only with GPVI in dimeric form and could be abrogated by pretreatment with collagen or CRP, implying at least partial overlap of the binding site for these ligands, however, fibrin‐GPVI monomer interactions and separate CRP and fibrin binding sites were proposed in another study . Under certain experimental conditions and in collaboration with αIIbβ3, the fibrin monomer component fibrinogen also can engage GPVI . Understanding how these two GPVI ligands intersect and contribute to GPVI function is important, as selective disruption of one type of GPVI‐ligand interaction, either through competitive inhibition at the ligand‐binding site, or at the level of GPVI dimerization represents an enticing new approach to develop antiplatelet agents with minimal effects on hemostasis.…”

Section: Triggers Of Platelet Receptor Sheddingmentioning

confidence: 99%

“…108 Under certain experimental conditions and in collaboration with αIIbβ3, the fibrin monomer component fibrinogen also can engage GPVI. 33,34 Understanding how these two GPVI ligands intersect and contribute to GPVI function is important, as selective disruption of one type of GPVI-ligand interaction, either through competitive inhibition at the ligand-binding site, or at the level of GPVI dimerization represents an enticing new approach to develop antiplatelet agents with minimal effects on hemostasis.…”

Section: Exposure To Gpvi Ligandsmentioning

confidence: 99%

“…The cytoplasmic domain of FcRγ contains an immunoreceptor tyrosine activation motif (ITAM) and together the GPVI/FcRγ complex transmits ligand‐induced signalling events into the platelet by triggering phosphorylation of two tyrosine residues with the ITAM and subsequent activation of p72‐spleen tyrosine kinase (Syk) . Along with collagen, GPVI can bind laminin, fibrin, fibrinogen, histones, adiponectin, and the extracellular matrix metalloproteinase inducer (EMMPRIN) expressed on monocytes and leukocytes. Intact GPVI is also essential for efficient generation of thrombin at the platelet surface .…”

Section: Introductionmentioning

confidence: 99%

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Proteolytic processing of platelet receptors

Gardiner

2018

Research and Practice in Thrombosis and Haemostasis

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Essentials Metalloproteinases regulate release/shedding of bioactive membrane proteins.Shedding is critically important for normal cell function in the vasculature.Levels of platelet receptors GPIb‐IX‐V and GPVI are regulated by metalloproteolytic shedding.The premier platelet sheddases belong to the A Disintegrins And Metalloproteinase (ADAMs) family.Modulating ADAM activity may alter platelet adheso‐signalling receptor density and function. Platelets have a major role in hemostasis and an emerging role in biological processes including inflammation and immunity. Many of these processes require platelet adhesion and localization at sites of tissue damage or infection and regulated platelet activation, mediated by platelet adheso‐signalling receptors, glycoprotein (GP) Ib‐IX‐V and GPVI. Work from a number of laboratories has demonstrated that levels of these receptors are closely regulated by metalloproteinases of the A Disintegrin And Metalloproteinase (ADAM) family, primarily ADAM17 and ADAM10. It is becoming increasingly evident that platelets have important roles in innate immunity, inflammation, and in combating infection that extends beyond processes of hemostasis. This overview will examine the molecular events that regulate levels of platelet receptors and then assess ramifications for these events in settings where hemostasis, inflammation, and infection processes are triggered.

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Nanofiber Topographies Enhance Platelet‐Fibrinogen Scaffold Interactions

Kenny

Stamboroski

Taher

et al. 2022

Adv Healthcare Materials

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The initial contact with blood and its components, including plasma proteins and platelets, directs the body's response to foreign materials. Natural scaffolds of extracellular matrix or fibrin contain fibrils with nanoscale dimensions, but how platelets specifically respond to the topography and architecture of fibrous materials is still incompletely understood. Here, planar and nanofiber scaffolds are fabricated from native fibrinogen to characterize the morphology of adherent platelets and activation markers for phosphatidylserine exposure and α‐granule secretion by confocal fluorescence microscopy and scanning electron microscopy. Different fibrinogen topographies equally support the spreading and α‐granule secretion of washed platelets. In contrast, preincubation of the scaffolds with plasma diminishes platelet spreading on planar fibrinogen surfaces but not on nanofibers. The data show that the enhanced interactions of platelets with nanofibers result from a higher locally accessible surface area, effectively increasing the ligand density for integrin‐mediated responses. Overall, fibrinogen nanofibers direct platelets toward robust adhesion formation and α‐granule secretion while minimizing their procoagulant activity. Similar results on fibrinogen‐coated polydimethylsiloxane substrates with micrometer‐sized 3D features suggest that surface topography could be used more generally to steer blood‐materials interactions on different length scales for enhancing the initial wound healing steps.

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Immobilized fibrinogen activates human platelets through glycoprotein VI

Cited by 100 publications

References 52 publications

Platelet preparation for function testing in the laboratory and clinic: Historical and practical aspects

Platelet preparation for function testing in the laboratory and clinic: Historical and practical aspects

Proteolytic processing of platelet receptors

Nanofiber Topographies Enhance Platelet‐Fibrinogen Scaffold Interactions

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