TP Receptor Antagonism: A New Concept in Atherothrombosis and Stroke Prevention

Chamorro, Ángel

doi:10.1159/000209262

Cited by 56 publications

(44 citation statements)

References 46 publications

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“…TXA 2 pathway inhibitors include picotamide (a combined TXA 2 synthase inhibitor and TP receptor blocker), ridogrel (a combined TXA 2 synthase inhibitor and TP receptor blocker), ramatroban (a TP receptor inhibitor), NCX 4016 (a nitric oxidereleasing aspirin derivative), Si8886/terutroban (a TP receptor inhibitor), and EV-077 (a combined TXA 2 synthase inhibitor and TP receptor blocker). 59,60 Some of these agents have been tested in clinical settings. In a randomized trial of patients with diabetes mellitus and peripheral artery disease (PAD), picotamide reduced long term overall mortality, but not major cardiovascular events, compared with aspirin.…”

Section: Thromboxane a 2 Pathway Inhibitorsmentioning

confidence: 99%

New Directions in Antiplatelet Therapy

Ferreiro

Angiolillo

2012

Circ: Cardiovascular Interventions

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A therosclerosis is a chronic inflammatory process that is known to be the underlying cause of coronary artery disease (CAD). 1 In addition to being the first step of primary hemostasis, platelets play a pivotal role in the thrombotic process that follows rupture, fissure, or erosion of an atherosclerotic plaque. 2 Because atherothrombotic events are essentially platelet-driven processes, this underscores the importance of antiplatelet agents, which represent the cornerstone of treatment, particularly in the settings of patients with acute coronary syndromes (ACS) and undergoing percutaneous coronary intervention (PCI).Currently, there are 3 different classes of antiplatelet drugs that are approved for clinical use and recommended per guidelines for the treatment and prevention of ischemic events in the settings of ACS and PCI: (1) cycloxigenase-1 (COX-1) inhibitor: aspirin, (2) adenosine diphosphate (ADP) P2Y 12 receptor antagonists: ticlopidine, clopidogrel, prasugrel, and ticagrelor, and (3) glycoprotein IIb/IIIa inhibitors (GPI): abciximab, eptifibatide, and tirofiban. 3-6 GPIs currently are available only for parenteral administration, and therefore their use is limited only to the acute phase of treatment of ACS patients undergoing PCI. Oral antiplatelet agents, namely aspirin and P2Y 12 receptor inhibitors, are recommended for prevention of ischemic events in both the acute and long-term phases of treatment. For over a decade, dual antiplatelet therapy (DAPT) with aspirin and clopidogrel has been considered the standard of care in the setting of ACS and PCI. However, a considerable number of adverse ischemic events continue to occur with this DAPT regimen, which has led to the development of newer and more potent antiplatelet agents. The objective of the present manuscript is to provide an overview on the most recent advances of currently approved antiplatelet agents in the setting of ACS and PCI, as well as on emerging agents that are in clinical development (Figure 1). Other antiplatelet drugs that are available for clinical use, such as pentoxifylline, cilostazol, and dypirimidamole, but do not have an approved indication for patients with ACS or undergoing PCI, as well as advances in anticoagulant therapy, will not be discussed.

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Section: Thromboxane a 2 Pathway Inhibitorsmentioning

confidence: 99%

New Directions in Antiplatelet Therapy

Ferreiro

Angiolillo

2012

Circ: Cardiovascular Interventions

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“…Ezeknek további jelentőségük lehet a cukorbetegek thrombocytáinak célzott kezelésében. [149][150][151][152] Az aszpirinkezelés kiegészítése clopidogrellel vitathatatlan klinikai előnnyel jár akut coronariaszindróma, illetve PCI esetén (lásd a táblázatban), azonban továbbra is jelentős számban következnek be visszatérő cardiovascularis események. Egyre több bizonyíték szól amellett, hogy e korlátozott hatékonyság hátterében a válaszkészség egyéni variációi állnak, diabetes mellitusban szenvedő betegek esetében is.…”

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Diabetes and Antiplatelet Therapy in Acute Coronary Syndrome

2011

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“…To this end, TPR's clear role in normal hemostasis is supported by the finding that “patients” have a bleeding disorder as a result of a point mutation in the receptor protein 14, 15, 16. On the other hand, upregulated signaling through TPR has been implicated in the pathogenesis of multiple cardiovascular and thrombosis‐based diseases 17, 18, 19, 20. Consistent with this concept are clinical findings indicating that inhibition of platelet TXA 2 production provides therapy for thromboembolic diseases,21, 22, 23 which is the underlying rationale for the use of aspirin in such diseases 24, 25…”

Section: Introductionmentioning

confidence: 99%

Investigation of a Thromboxane A ₂ Receptor–Based Vaccine for Managing Thrombogenesis

Alshbool

Karim

Espinosa

et al. 2018

JAHA

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BackgroundDespite the well‐established role for the thromboxane A2 receptor (TPR) in the development of thrombotic disorders, none of the antagonists developed to date has been approved for clinical use. To this end, we have previously shown that an antibody targeted against TPR's ligand‐binding domain inhibits platelet activation and thrombus formation, without exerting any effects on hemostasis. Thus, the goal of the present studies is to design a novel TPR‐based vaccine, demonstrate its ability to trigger an immune response, and characterize its antiplatelet and antithrombotic activity.Methods and ResultsWe used a mouse keyhole limpet hemocyanin/peptide‐based vaccination approach rationalized over the TPR ligand‐binding domain (ie, the C‐terminus of the second extracellular loop). The biological activity of this vaccine was assessed in the context of platelets and thrombotic diseases, and using a host of in vitro and in vivo platelet function experiments. Our results revealed that the TPR C‐terminus of the second extracellular loop vaccine, in mice: (1) triggered an immune response, which resulted in the development of a C‐terminus of the second extracellular loop antibody; (2) did not affect expression of major platelet integrins (eg, glycoprotein IIb‐IIIa); (3) selectively inhibited TPR‐mediated platelet aggregation, platelet‐leukocyte aggregation, integrin glycoprotein IIb‐IIIa activation, as well as dense and α granule release; (4) significantly prolonged thrombus formation; and (5) did so without impairing physiological hemostasis.ConclusionsCollectively, our findings shed light on TPR's structural biological features, and demonstrate that the C‐terminus of the second extracellular loop domain may define a new therapeutic target and a TPR vaccine‐based approach that should have therapeutic applications.

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TP Receptor Antagonism: A New Concept in Atherothrombosis and Stroke Prevention

Cited by 56 publications

References 46 publications

New Directions in Antiplatelet Therapy

New Directions in Antiplatelet Therapy

Diabetes and Antiplatelet Therapy in Acute Coronary Syndrome

Investigation of a Thromboxane A ₂ Receptor–Based Vaccine for Managing Thrombogenesis

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TP Receptor Antagonism: A New Concept in Atherothrombosis and Stroke Prevention

Cited by 56 publications

References 46 publications

New Directions in Antiplatelet Therapy

New Directions in Antiplatelet Therapy

Diabetes and Antiplatelet Therapy in Acute Coronary Syndrome

Investigation of a Thromboxane A 2 Receptor–Based Vaccine for Managing Thrombogenesis

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Product

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Investigation of a Thromboxane A ₂ Receptor–Based Vaccine for Managing Thrombogenesis