Factor XIII improves platelet adhesion to fibrinogen by protein disulfide isomerase-mediated activity

Lahav, Judith; Tvito, Ariella; Bagoly, Zsuzsa; Dardik, Rima; Inbal, Aida

doi:10.1016/j.thromres.2012.12.003

Cited by 7 publications

(4 citation statements)

References 23 publications

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“…Although multiple mechanisms alter platelet function in the context of liver regeneration [39], FXIII-induced cross-linking stabilizes fibrin [40], and this may be critical to drive platelet accumulation in the early moments after PHx. Moreover, multiple studies have shown that FXIII directly contributes to platelet adhesion to fibrin and drives platelet responses secondary to fibrin(ogen)-integrin α IIb β 3 engagement [41][42][43]. In addition to platelets, fibrin engagement of leukocyte β2 integrins [44] could contribute to liver regeneration by modulating effector functions of either neutrophils or macrophages, both cell types linked to liver regeneration in mice and humans [45,46].…”

Section: Impact Of Fxiii Deficiency On Hepatocyte Proliferation After...mentioning

confidence: 99%

Coagulation factor XIII is a critical driver of liver regeneration after partial hepatectomy

Wei,

Groeneveld,

Adelmeijer

et al. 2024

Journal of Thrombosis and Haemostasis

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Section: Impact Of Fxiii Deficiency On Hepatocyte Proliferation After...mentioning

confidence: 99%

Coagulation factor XIII is a critical driver of liver regeneration after partial hepatectomy

Wei,

Groeneveld,

Adelmeijer

et al. 2024

Journal of Thrombosis and Haemostasis

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“…Cell surface receptors can be activated via binding, but also through cleavage by proteases; kallekrein-14 and cathepsin G are PDI substrates and are known to cleave and activate members of the PAR receptor family (8, 39, 40). PDI can modulate phosphatidylserine (PS) exposure (16, 41) and may regulate coagulation through disulfide regulation of tissue factor, activation of factor XI, maturation of platelet factor V, and attenuating factor XIII cross-linking activity toward fibrin (8, 9, 13, 42, 43). More globally, PDI is believed to sense and regulate the redox state of the extracellular membrane, by interacting with small molecule effectors like glutathione and nitric oxide (NO), and modulating the redox state of other extracellular thiol isomerases (5, 6, 44).…”

Section: Pdi and Thrombus Formationmentioning

confidence: 99%

“…Interaction with either of these receptors leads to platelet activation which can enhance the metastatic potential of the tumor through shielding from an anti-tumor immune response (59, 60, 62). Several cell surface receptors, receptor agonist proteases, and large scaffolding proteins which bind to these receptors across multiple cells and strengthen the thrombus have all been identified as PDI substrates (9, 12, 14, 33, 35, 38, 43).…”

Section: Hypercoagulability Of Cancer and Potential Interface With Pdimentioning

confidence: 99%

The intersection of protein disulfide isomerase and cancer associated thrombosis

Stopa¹,

Zwicker²

2018

Thrombosis Research

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The mechanisms underlying the hypercoagulability of cancer are complex and include the upregulation coagulation factors or procoagulant proteins, shedding of microparticles, and direct activation of vascular cells. Protein disulfide isomerase (PDI) is a thiol isomerase secreted from activated platelets and endothelial cells and plays a critical role in both platelet aggregation and fibrin generation. A number of potential intravascular targets of PDI have been identified including cell surface receptors (e.g. β-integrins and glycoprotein Ib), receptor ligands (e.g. fibrinogen and von Willebrand factor), serine proteases (e.g. cathepsin G and kallekrein-14), and coagulation factors (e.g. factor XI and factor V). Recent clinical studies demonstrated that a small molecule inhibitor of PDI, isoquercetin, decreases platelet-dependent thrombin generation and PDI activity in plasma following oral administration. This review explores the mechanistic overlap between the molecular drivers of cancer associated thrombosis and the potential roles PDI plays in mediating thrombosis. These molecular insights provide rationale for clinical trials targeting PDI to prevent thrombosis in cancer patients.

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“…Это может быть одной из причин тромбозов при АФС. Также показано, что фактор XIII (FXIII; его А-цепь) обладает активностью ПДИ, и тем самым способствует адгезии и агрегации тромбоцитов [43,44].…”

Section: Thiol Isomerases As a Target For Antithrombotic Therapy тиолunclassified

Thiol Isomerases – A Possible Target for Thrombosis Control

Gribkova¹,

Davydovskaya

2017

Racionalʹnaâ farmakoterapiâ v kardiologii

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1 Центр клинических исследований и оценки медицинских технологий, Департамент здравоохранения г. Москвы. Россия, 121096, Москва, ул. Минская, 12 корп. 2 2 Российский национальный исследовательский медицинский университет имени Н.И. Пирогова Россия, 117997, Москва, ул. Островитянова, 1Несмотря на то, что растет количество антитромботических агентов с подтвержденной клинической эффективностью, тромбозы остаются ве-дущей причиной смертности в развитых странах. Поэтому существует необходимость в разработке новых видов терапии с использованием альтернативных мишеней компонентов свертывания крови на основе новых знаний о механизмах тромбообразования. Благодаря новым ме-тодам и подходам к исследованию этих механизмов в последнее время неожиданно было открыто, что в процессы тромбообразования во-влечены внеклеточные тиоловые изомеразы. Протеин дисульфид изомераза (ПДИ) выделяется из тромбоцитов и эндотелиальных клеток после активации и локализуется на поверхности мембраны. Учитывая роль ПДИ в регулировании как агрегации тромбоцитов, так и генерации фиб-рина in vivo, обсуждается возможность использования ПДИ в качестве антитромботической мишени. Тогда как большинство существующих антитромботических средств направлены либо против агрегации тромбоцитов, либо против активации плазменного свертывания, ингиби-торы ПДИ имеют потенциал для предупреждения тромбозов в условиях патологической активации обоих путей, вовлеченных в сложные тром-ботические заболевания, такие как инфаркт миокарда и тромбозы, связанные с онкологическими заболеваниями. В обзоре рассмотрены по-следние данные о роли ПДИ в формировании тромба, основные мишени и механизмы действия, а также ингибиторы ПДИ как кандидаты на новый класс антитромботической терапии с антиагрегантной и антикоагулянтной активностью для предотвращения тромбообразования в организме человека. While there are an increasing number of antithrombotic agents with demonstrated clinical efficacy, thrombosis remains the leading cause of mortality in developed countries. Therefore, there is a need further development of therapies targeting alternative components of the blood clotting mechanism, based on new knowledge about the mechanisms of thrombus formation. Recently, among several unexpected findings of new methods and approaches to the study of these mechanisms it was discovered that protein disulfide isomerase (PDI) serves an essential role in the processes of thrombus formation. PDI is secreted by platelets and endothelial cells following activation and localizes to the membrane surface. Given the role of PDI in regulating both platelet aggregation and fibrin generation in vivo, the possibility of using PDI as an antithrombotic target is discussed. While most antithrombotic target either platelet or coagulation activation, PDI inhibitors have the potential to prevent thrombosis in conditions with pathologic activation of both pathways as implicated in complex thrombotic disorders such as myocardial infarction and cancer associated thrombosis. This review considers what is known about the ...

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Factor XIII improves platelet adhesion to fibrinogen by protein disulfide isomerase-mediated activity

Cited by 7 publications

References 23 publications

Coagulation factor XIII is a critical driver of liver regeneration after partial hepatectomy

Coagulation factor XIII is a critical driver of liver regeneration after partial hepatectomy

The intersection of protein disulfide isomerase and cancer associated thrombosis

Thiol Isomerases – A Possible Target for Thrombosis Control

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