Altered plasma fibrin clot properties in essential thrombocythemia

Małecki, Rafał; Gacka, Małgorzata; Kuliszkiewicz‐Janus, Małgorzata; Jakobsche-Policht, Urszula; Kwiatkowski, J; Adamiec, Rajmund; Undas, Anetta

doi:10.3109/09537104.2015.1042967

Cited by 15 publications

(16 citation statements)

References 38 publications

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“…Soluble P‐selectin promotes NET formation . Moreover, the associations between sP‐selectin and both K s and CLT support growing evidence for the impact of platelet‐derived proteins on clot properties reported previously …”

Section: Discussionsupporting

confidence: 85%

“…40 Moreover, the associations between sP-selectin and both K s and CLT support growing evidence for the impact of platelet-derived proteins on clot properties reported previously. 41 We confirmed that older age 42 and higher platelet count 7 can predict cancer diagnosis following unprovoked VTE. We did not find male sex to be a risk factor, as opposed to the studies by Jara-Palomares et al 7 and Rieu et al, 43 although evidence for this issue is inconsistent.…”

Section: Discussionsupporting

confidence: 69%

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Prothrombotic fibrin clot properties associated with increased endogenous thrombin potential and soluble P‐selectin predict occult cancer after unprovoked venous thromboembolism

Mrozińska

Cieślik

Broniatowska

et al. 2019

Journal of Thrombosis and Haemostasis

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Background Compact fibrin clots relatively resistant to lysis are observed in patients at increased risk of venous thromboembolism (VTE) including malignancy. The citrullinated histone H3 (H3Cit) predicts VTE in cancer patients. Objectives We performed a cohort study to investigate whether abnormal clot properties predict cancer diagnosis following unprovoked VTE. Methods In 369 consecutive patients aged <70 years without malignancy detected during routine screening, we determined plasma clot permeability (Ks) and clot lysis time (CLT), along with several prothrombotic markers and H3Cit after 2 to 8 months since VTE. Results During follow‐up (median, 37; interquartile range, 33‐39 months), malignancy was diagnosed in 22 patients (6%), who were older. This group had denser fibrin networks (−13% Ks), impaired fibrinolysis (+25.5% CLT), increased endogenous thrombin potential (ETP,+7%), soluble P‐selectin (+40.3%), and H3Cit (+169.2%) measured off anticoagulation after median 4 months since VTE. The Ks and CLT correlated with H3Cit (r = −.58 and r = .31, P < .05, respectively). The Kaplan–Meier survival analysis showed that reduced Ks (the first quartile, ≤6.2 × 10−9 cm2), prolonged CLT (the top quartile, >106 min), and higher ETP (the top quartile, >1657 nM × min) were predictors of cancer diagnosed during follow‐up. The multivariable Cox proportional hazards model showed that patients with the prothrombotic clot phenotype (low Ks and long CLT) had the highest risk of cancer diagnosis [hazard ratio(HR), 23.4; 95% confidence interval (CI), 6.67‐82.15]. Conclusions Prothrombotic clot properties following unprovoked VTE might help identify patients at risk of a diagnosis of cancer within the first 3 years of follow‐up.

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Section: Discussionsupporting

confidence: 85%

Section: Discussionsupporting

confidence: 69%

Prothrombotic fibrin clot properties associated with increased endogenous thrombin potential and soluble P‐selectin predict occult cancer after unprovoked venous thromboembolism

Mrozińska

Cieślik

Broniatowska

et al. 2019

Journal of Thrombosis and Haemostasis

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“…Several studies indicate that K s measurement might be a suitable tool for clinical use; however, differences in the results, given the use of various concentrations of reagents and techniques in laboratories, limit its current applicability and require further efforts to standardize this technique, which has huge potential clinical implications. Prospective studies are Atherosclerotic vascular diseases Stable coronary artery disease, 48 peripheral arterial disease 49 Thromboembolic arterial events Acute coronary syndromes, 28 no-reflow phenomenon after acute MI, 50 instent thrombosis, 51 previous ischemic stroke, 29 acute ischemic stroke 52 Other cardiovascular diseases Chronic heart failure with sinus rhythm, 53 atrial fibrillation (paroxysmal, persistent, and permanent), 37,54 arterial hypertension 55 Venous thrombosis Idiopathic venous thromboembolism, 56 cerebral venous sinus thrombosis 57 Chronic renal disease End-stage renal disease on peritoneal dialysis 58 and long-term hemodialysis 59 Malignancy Digestive tract cancer, 60 multiple myeloma, 61 essential thrombocythemia 62 Autoimmune or chronic inflammatory diseases Inflammatory bowel disease, 63 antiphospholipid syndrome, 64,65 rheumatoid arthritis 66 Other Factor XIII Val34Leu polymorphism, 67 elevated plasma lipoprotein(a), 68 familial history of premature coronary artery disease 27 or venous thromboembolism 69 Increased K s…”

Section: Resultsmentioning

confidence: 99%

How to Assess Fibrinogen Levels and Fibrin Clot Properties in Clinical Practice?

Undas

2016

Semin Thromb Hemost

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Fibrin formed from fibrinogen is the main component of thrombi. Clot structure is characterized by fiber thickness and pore size, which differs within a given clot and between individuals. Plasma clot architecture is largely determined by the quantity and quality of fibrinogen. Plasma fibrinogen concentrations are most commonly measured in citrated plasma using the Clauss method. However, several factors, including instrument type and reagent, may affect results. Other approaches to express the ability of fibrinogen to clot involve prothrombin time-derived or clottable protein assays, while fibrinogen antigen levels in clinical settings are measured using immunological or precipitation assays. Fibrin clot permeability (reflected by the Darcy constant, K s) being proportional to a buffer volume percolating through a clot under a given hydrostatic pressure is now the most commonly used measure of clot structure. Low K s values indicating tightly packed fibrin structure have been shown to be associated with venous and arterial thrombotic complications, while high K s might contribute to bleeding disorders. The measurement of K s, however, is not standardized and validated. This review summarizes the current knowledge on practical aspects of the measurement of fibrinogen levels and K s in patients.

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“…The structure of fibrin networks is often affected by physical factors, such as hydrodynamic flow or a strong magnetic field that result in formation of oriented anisotropic fibrin fibers (Gersh et al 2010; Campbell et al 2010). Fibrin structure and properties are greatly influenced by the presence of blood cells, namely activated platelets and erythrocytes (Aleman et al 2014; Malecki et al 2015) that form a natural and very active environment for clot formation. In addition to whole cells, the effects of circulating cell-derived microparticles on the fibrin clot structure and properties have been recently demonstrated (Zubairova et al 2015).…”

Section: 4 Variations and Modulation Of Fibrin(ogen) Structure Andmentioning

confidence: 99%

Fibrin Formation, Structure and Properties

Weisel

Litvinov

2017

Subcellular Biochemistry

512

498

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Fibrinogen and fibrin are essential for hemostasis and are major factors in thrombosis, wound healing, and several other biological functions and pathological conditions. The X-ray crystallographic structure of major parts of fibrin(ogen), together with computational reconstructions of missing portions and numerous biochemical and biophysical studies, have provided a wealth of data to interpret molecular mechanisms of fibrin formation, its organization, and properties. On cleavage of fibrinopeptides by thrombin, fibrinogen is converted to fibrin monomers, which interact via knobs exposed by fibrinopeptide removal in the central region, with holes always exposed at the ends of the molecules. The resulting half-staggered, double-stranded oligomers lengthen into protofibrils, which aggregate laterally to make fibers, which then branch to yield a three-dimensional network. Much is now known about the structural origins of clot mechanical properties, including changes in fiber orientation, stretching and buckling, and forced unfolding of molecular domains. Studies of congenital fibrinogen variants and post-translational modifications have increased our understanding of the structure and functions of fibrin(ogen). The fibrinolytic system, with the zymogen plasminogen binding to fibrin together with tissue-type plasminogen activator to promote activation to the active proteolytic enzyme, plasmin, results in digestion of fibrin at specific lysine residues. In spite of a great increase in our knowledge of all these interconnected processes, much about the molecular mechanisms of the biological functions of fibrin(ogen) remains unknown, including some basic aspects of clotting, fibrinolysis, and molecular origins of fibrin mechanical properties. Even less is known concerning more complex (patho)physiological implications of fibrinogen and fibrin.

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Altered plasma fibrin clot properties in essential thrombocythemia

Cited by 15 publications

References 38 publications

Prothrombotic fibrin clot properties associated with increased endogenous thrombin potential and soluble P‐selectin predict occult cancer after unprovoked venous thromboembolism

Prothrombotic fibrin clot properties associated with increased endogenous thrombin potential and soluble P‐selectin predict occult cancer after unprovoked venous thromboembolism

How to Assess Fibrinogen Levels and Fibrin Clot Properties in Clinical Practice?

Fibrin Formation, Structure and Properties

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