Structural studies of factor XIII /

Fox, Brian Andrew.

January 2000

Thesis (Ph. D.)--University of Washington, 2000. / Vita. Includes bibliographical references (leaves 90-101).

Factor XIII Factor XIII

Mechanisms Coupling Hemostatic Factors to Inflammatory Arthritis

Raghu, Harini

10 October 2014

No description available.

Immunology

Hemostasis

Arthritis

Inflammation

Factor XIII

Plasminogen

Fibrinogen

Avaliação de alguns parametros da fibrinolise e do fator XIII em pacientes com trombose venosa profunda espontanea e doença hemorragica / Evaluation of fibrinolysis and factor XIII some parameters in patients with spontaneous deep venous trombosis and hemorrhagic disease

Araujo, Graziela Silveira

13 March 2008

Orientador: Joyce Maria Annichino-Bizzacchi / Dissertação (mestrado) - Universidade Estadual de Campinas, Faculdade de Ciencias Medicas / Made available in DSpace on 2018-08-11T06:35:03Z (GMT). No. of bitstreams: 1 Araujo_GrazielaSilveira_M.pdf: 2289744 bytes, checksum: 6cde67a2a95fde59c04e1240833b9c41 (MD5) Previous issue date: 2008 / Resumo: Em uma parcela de pacientes com quadro clínico hemorrágico ou trombótico, nenhum diagnóstico etiológico é estabelecido. Os pacientes com doença hemorrágica, muitas vezes importante, podem apresentar todos os exames de triagem e dosagem específica de fatores da coagulação dentro dos valores da normalidade. OBS.: O resumo na integra poderá ser visualizado no link ou texto completo da tese digital / Abstract: In a parcel of patients with hemorrhagic or thrombotic clinical picture, none etiologic diagnosis is established. The patients with hemorrhagic desorder, many times important, can present all inside the screening tests and specific dosage of factors of the coagulation of the values of normality. Note: the complete abstract is avaiable with the link or full eletronic digital theses or dissertations / Mestrado / Biologia Estrutural, Celular, Molecular e do Desenvolvimento / Mestre em Fisiopatologia Médica

Fibrinólise

Transtornos hemostaticos

Trombose venosa

Deficiência do fator XIII

Fibrinolysis

Hemostatic disorders

Venous thrombosis

Factor XIII deficiency

Free oscillation rheometry monitoring of haemodilution and hypothermia and correction with fibrinogen and factor XIII concentrates

Winstedt, Dag, Tynngård, Nahreen, Olanders, Knut, Schott, Ulf

January 2013

Background Haemodilution and hypothermia induce coagulopathy separately, but their combined effect on coagulation has not been widely studied. Fibrinogen concentrate can correct dilutional coagulopathy and has an additional effect when combined with factor XIII concentrate. However, their effect on dilutional coagulopathy concomitant with hypothermia has not been studied previously. Free oscillation rheometry – FOR (Reorox®) – is a novel viscoelastic haemostatic assay that has not been studied in this context before. Methods Blood from 10 healthy volunteers was diluted by 33% with hydroxyethyl starch or Ringer’s acetate solutions. Effects of fibrinogen added in vitro with and without factor XIII were studied at 33°C and 37°C. Coagulation velocity (coagulation time) and clot strength (elasticity) were assessed with FOR. Coagulation was initiated in vitro with thromboplastin alone, or thromboplastin plus a platelet inhibitor. Results Hydroxyethyl starch increased the coagulation time and decreased clot strength significantly more than Ringer’s acetate solution, both in the presence and absence of a platelet inhibitor. There was a significant interaction between haemodilution with hydroxyethyl starch and hypothermia, resulting in increased coagulation time. After addition of fibrinogen, coagulation time shortened and elasticity increased, with the exception of fibrinogen-dependent clot strength (i.e., elasticity in the presence of a platelet inhibitor) after hydroxyethyl starch haemodilution. Factor XIII had an additional effect with fibrinogen on fibrinogen-dependent clot strength in blood diluted with Ringer’s acetate solution. Hypothermia did not influence any of the coagulation factor effects. Conclusions Both haemodilution and mild hypothermia impaired coagulation. Coagulopathy was more pronounced after haemodilution with hydroxyethyl starch than with Ringer’s acetate. Addition of fibrinogen with factor XIII was unable to reverse hydroxyethyl starch induced clot instability, but improved coagulation in blood diluted with Ringer’s acetate solution. Fibrinogen improved coagulation irrespective of hypothermia. / <p>Funding Agencies|Region Skane (Sweden)||CSL Beehring||</p>

Free oscillation rheometry

Thrombelastography

Coagulation factor concentrate

Fibrinogen

Factor XIII

Haemodilution

Hypothermia

Coagulopathy

Hydroxyethyl starch

Ringers acetate solution

MEDICINE

MEDICIN

Étude des facteurs de l'hémostase après thrombolyse par le rT-PA dans l'infractus cérébral aigu : corrélations cliniques et étiologiques / Haemostasis factors after rt-PA thrombolysis in acute cerebral infarct

Sun, Xuhong

15 September 2015

L'étude systématique de l'hémostase post-thrombolytique a été peu étudiée. Chez 80 malades thrombolysés consécutifs, une étude prospective a comporté l'étude – aux heures 0, 2 et 24 – des facteurs de l'hémostase suivants: fibrinogène, plasminogène, PDF (produits de dégradation de la fibrine et du fibrinogène), D-dimères, alpha2-antiplasmine et facteur XIII, ainsi que l'hématocrite et la numération plaquettaire. Des calculs statistiques approfondis ont exploré les corrélations des variations des facteurs hémostatiques entre eux et avec 37 paramètres cliniques et étiologiques. Processus moléculaires post-thrombolytiques. Le rt-PA induit deux processus, indépendants statistiquement à la 2ème heure: d'une part une élévation des PDF et des D-dimères; d'autre part, une baisse du fibrinogène, corrélée à une baisse du plasminogène (r=0,48, p=0.01), de l'alpha2-antiplasmine (r=0.48, p =0.004) et du facteur XIII (r=0.44, p=0.01). La baisse du plasminogène est corrélée significativement avec celle de l'alpha2-antiplasmine (r=0.77, p<0.001), et du facteur XIII (r=0.47, p=0.02). La mise en jeu de facteurs anti-fibrinolytiques, qui n'avait jamais été décrite précédemment, peut jouer un rôle dans une limitation de la fibrinolyse et dans la rethrombose. Des corrélations sont notées entre la baisse précoce du plasminogène et l'étiologie cardioembolique (p=0.04), et un mauvais pronostic final (p=0.03), possiblement en rapport la thrombolyse intense de gros caillots. Les hématomes intra-cérébraux parenchymateux (HP) sont liés significativement à la baisse du fibrinogène (p=0.01) et à l'augmentation des PDF (p=0.01). Une baisse du fibrinogène au-dessous de 2g/L multiplie la probabilité de HP précoce par un facteur 12,82. Ainsi est confirmé le modèle d'une “coagulopathie précoce avec dégradation du fibrinogène”», prédictive de l'hématome, proposé par l'équipe lyonnaise de thrombolyse en 2004 / A systematic study of post-thrombolytic haemostasis has rarely been performed. In 80 consecutive patients, we have prospectively studied at hours 0, 2 and 24 the following parameters: fibrinogen, plasminogen, alpha2-antiplasmin, factor XIII, fibrin(ogen) Degradation Products (FDP), D-dimers, haematocrit and platelet count. Comprehensive statistical studies calculated correlations of the haemostatic values betwen themselves and with 38 etiological and clinical parameters. Molecular dynamics. Two changes between h0 and h2 were statistically independent: an increase in FDP and D-Dimers; a decrease in fibrinogen, plasminogen, alpha2-antiplasmin and factor XIII. At h2, the decrease in fibrinogen was significantly correlated with that of plasminogen (0.48, p = 0.01), alpha2-antiplasmin (0.48, p = 0.004), and factor XIII (0.44, p = 0.01). The decrease in plasminogen was significantly correlated with those of antifibrinolytic components, alpha2-antiplasmin (r=0.77, p<0.001) and factor XIII (0.47, p=0.02). To our knowledge, such an activation of antifibrinolytic components had not hitherto been mentioned. The h2 decrease of plasminogen was correlated with cardioembolic etiology (p=0.04) and final poor oucome (p=0.03), a fact possibly due to intense thrombolysis of large clots. Patients having early parenchymal hematomas (PH) showed h2 haemostasis disturbances: high FDP (p=0.01), and low fibrinogen (p=0.01). The decrease in fibrinogen less than 2g/L multiplies the odds of early PH by a factor 12.82. Thus, we confirm the model of an “early fibrinogen degradation coagulopathy” predictive of hematomas, which had been coined by the Lyon thrombolysis team in 2004

Thrombolyse

Rt-PA

Fibrinogène

Plasminogène

Alpha2-antiplasmine

Facteur XIII

D-dimères

Thrombolysis

Rt-PA

Fibrinogen

Plasminogen

Alpha2-antiplasmin

Factor XIII

Fibrin(ogen) Degradation Products (FDP)

D-dimers

612.8