A Role of the Fast ATP-gated P2X1 Cation Channel in Thrombosis of Small Arteries In Vivo

Hechler, Béatrice; Lenain, Nadège; Marchese, Patrizia; Vial, Céline; Heim, Véronique; Freund, Monique; Cazenave, Jean‐Pierre; Cattaneo, Marco; Ruggeri, Zaverio M.; Evans, Richard J.; Gachet, Christian

doi:10.1084/jem.20030144

Cited by 191 publications

(241 citation statements)

References 25 publications

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“…Although unable to trigger platelet aggregation by itself, the P2X 1 receptor induces transient shape change [13] and participates in collagenand shear-induced aggregation [86][87][88]. A comprehensive review of its role in platelet function is provided by Martyn Mahaut-Smith (this issue).…”

Section: Receptormentioning

confidence: 99%

“…In contrast, they display resistance to the systemic thromboembolism induced by injection of a mixture of collagen and adrenaline and to localized laser-induced injury of the vessel wall of mesenteric arteries [88]. Since in vitro the P2X 1 receptor plays an important role in thrombus formation only under high shear conditions, it might represent the ideal target for an antithrombotic drug.…”

Section: The P2y 1 Receptor As a Target For New Antiplatelet Compoundsmentioning

confidence: 99%

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P2 receptors and platelet function

Hechler

Gachet

2011

Purinergic Signalling

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Following vessel wall injury, platelets adhere to the exposed subendothelium, become activated and release mediators such as TXA 2 and nucleotides stored at very high concentration in the so-called dense granules. Released nucleotides and other soluble agents act in a positive feedback mechanism to cause further platelet activation and amplify platelet responses induced by agents such as thrombin or collagen. Adenine nucleotides act on platelets through three distinct P2 receptors: two are G proteincoupled ADP receptors, namely the P2Y 1 and P2Y 12 receptor subtypes, while the P2X 1 receptor ligand-gated cation channel is activated by ATP. The P2Y 1 receptor initiates platelet aggregation but is not sufficient for a full platelet aggregation in response to ADP, while the P2Y 12 receptor is responsible for completion of the aggregation to ADP. The latter receptor, the molecular target of the antithrombotic drugs clopidogrel, prasugrel and ticagrelor, is responsible for most of the potentiating effects of ADP when platelets are stimulated by agents such as thrombin, collagen or immune complexes. The P2X 1 receptor is involved in platelet shape change and in activation by collagen under shear conditions. Each of these receptors is coupled to specific signal transduction pathways in response to ADP or ATP and is differentially involved in all the sequential events involved in platelet function and haemostasis. As such, they represent potential targets for antithrombotic drugs.

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Section: Receptormentioning

confidence: 99%

Section: The P2y 1 Receptor As a Target For New Antiplatelet Compoundsmentioning

confidence: 99%

P2 receptors and platelet function

Hechler

Gachet

2011

Purinergic Signalling

Self Cite

136

127

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“…This aggregation was found to require von Willebrand factor multimers, extracellular calcium (Ca 2+ ), ADP released from the platelets, fibrinogen, and platelet membrane glycoproteins GPIbα and αIIbβ3 [71,72]. More recently, the P2X 1 receptor, stimulated by ATP released from platelets, has been shown to be required for shear-induced aggregation [73][74][75]. It has also now been found that blocking the P2Y 1 receptor for ADP prevents stabilization of aggregation [76,77].…”

Section: Role Of Adp In Shear-induced Aggregationmentioning

confidence: 99%

“…They used transgenic mice overexpressing the P2X 1 receptor in the megakaryocyte cell lineage and found that their platelets showed enhanced aggregation and secretion in response to collagen, compared with platelets from wild-type mice. Hechler and colleagues [75] showed that platelets from mice deficient in the P2X 1 receptor had a decreased aggregation response to collagen and were protected from arterial thrombosis.…”

Section: The P2x 1 Receptormentioning

confidence: 99%

Historical perspective on ADP-induced platelet activation

Packham

Rand

2011

Purinergic Signalling

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“…Platelet activation by ATP amplifies the platelet responses to other agonists, especially in flow conditions that are characterized by high shear stress [18][19][20][21][22].…”

mentioning

confidence: 99%

Molecular defects of the platelet P2 receptors

Cattaneo

2011

Purinergic Signalling

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Human platelets express three types of P2 receptors, which play important roles in platelet function: P2X 1 , P2Y 1 and P2Y 12 . Only patients with either quantitative or qualitative abnormalities of the platelet P2Y 12 receptor have been well-characterized so far. Deficiencies of P2Y 12 are associated with nucleotide deletions in the open-reading frame, frameshifts, and early truncation of the protein, or with a nucleotide substitution in the transduction initiation codon. Congenital dysfunctions of P2Y 12 are associated with molecular defects involving the sixth trans-membrane domain or the adjacent third extracellular loop of the receptor, which identify a region of the protein whose integrity is necessary for normal receptor function. A mutation, predicting a lysine to glutamate (Lys174Glu) substitution was associated with decreased ligand binding to the receptor, suggesting that it is responsible for disruption of the adenosine diphosphate (ADP)-binding site of the receptor. Patients with P2Y 12 defects display a mild-tomoderate bleeding diathesis, characterized by mucocutaneous bleedings and excessive post-surgical and posttraumatic blood loss. Defects of P2Y 12 should be suspected when ADP, even at high concentrations (≥10 μM), is unable to induce full, irreversible platelet aggregation. Tests that evaluate the degree of inhibition of adenylyl cyclase by ADP should be used to confirm the diagnosis.

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A Role of the Fast ATP-gated P2X1 Cation Channel in Thrombosis of Small Arteries In Vivo

Cited by 191 publications

References 25 publications

P2 receptors and platelet function

P2 receptors and platelet function

Historical perspective on ADP-induced platelet activation

Molecular defects of the platelet P2 receptors

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