Avaliação da hemostasia na Doença de Crohn subclínica: papel da atividade endoscópica / Hemostatic parameters in Crohn\'s Disease in clinical remission: role of endoscopic activity

Andrade, Adriana Ribas

25 July 2018

Introdução: Pacientes com Doença de Crohn (DC) apresentam alto risco de eventos tromboembólicos (TE), muitas vezes, associados a alta morbimortalidade. É conhecido o papel da inflamação na fisiopatologia da trombose na doença Inflamatória Intestinal (DII), entretanto, o significado da inflamação subclínica ainda se mantém obscuro na literatura. Este estudo avaliou o efeito da atividade endoscópica no perfil de coagulação dos pacientes com DC em remissão clínica. Métodos: entre os dias 22 de maio de 2015 e 26 de abril de 2017, foram triados 261 pacientes com DC em possível remissão clínica, sendo realizadas ao todo 229 colonoscopias. Das 229 colonoscopias realizadas, 164 pacientes estavam realmente em remissão clínica (confirmados com CDAI <= 150) e foram alocados em dois grupos: 75 no grupo de atividade endoscópica (AE) (SES-CD >= 7), 89 no grupo de remissão endoscópica (RE) (SES-CD <= 2). Cinquenta controles saudáveis pareados por sexo e idade foram eleitos. Medimos, nos 3 grupos, além da geração de trombina - pelo método Calibrated Automated Thrombogram (CAT), com e sem trombomodulina, - a atividade do fator tecidual (FT), fibrinogênio, D-dímero, Fator VIII, ADAMTS-13, Fator de von Willebrand - antígeno e cofator de ristocetina (cWF). Coletamos dados sobre a duração da doença, extensão, comportamento, localização, tratamento farmacológico, história prévia de cirurgias, calprotectina fecal, qualidade de vida (por meio do IBDQ), além dos fatores de risco para TE, como hospitalização recente, uso de corticoide atual, status do tabagismo, assim como marcadores de trombofilia hereditária ou adquirida. Seguimos os pacientes por 1 ano de observação, avaliando a variação no CDAI e IBDQ no período. Resultados: A maioria dos pacientes apresentou comprometimento ileocolônico (43%), com comportamento inflamatório (40%), seguido de estenosante (30%) e fistulizante (30%). 67% estavam em uso de imunossupressores e 52% em uso de biológicos. Os fatores de risco para TE e todos os outros marcadores de trombofilia, incluindo deficiência de proteína C e S, anticardiolipina, resistência à proteína C, antitrombina, mutações da protrombina e do Fator V, foram semelhantes em ambos os grupos, exceto pelo anticoagulante lúpico, maior no grupo de AE (8,1% vs. 1,3%, p=0,047). Como esperado, o grupo de AE apresentou níveis significativamente maiores de PCR, calprotectina fecal e plaquetas. Além disso, este grupo apresentou uma maior atividade do fator tecidual vs. o grupo de RE vs. controles (127 vs. 103 vs. 84, p = 0,001). Embora o grupo DC tivesse maiores níveis de FVW:Ag e FVW:RCo, FVW/ADAMTS-13, Fator VIII e trombomodulina vs. controles, não houve diferença estatística entre os grupos de AE e RE. Os níveis de geração de trombina foram semelhantes entre os 3 grupos, com ou sem trombomodulina. Conclusão: Esses dados evidenciam que existe uma disfunção endotelial inerente à DC, e, que, em pacientes com AE, essa disfunção pode ser ainda maior pela maior exposição do FT. Embora, a presença de inflamação e dano endotelial contribuam para esse estado procoagulante, em pacientes com doença subclínica, há um estado de compensação permanente, uma vez que a quantidade de trombina gerada foi a mesma entre os grupos. Este equilíbrio pode estar comprometido diante de outros fatores tromboembólicos, aumentando, assim, o risco de trombose / Background: Crohn\'s disease patients (CD) have a high risk of thromboembolic events (TE), often associated with high morbidity and mortality. Involvement of inflammation in TE is well known, but significance of the sub-clinical inflammation in this process is not the rule. Thus, the aim of this study is to evaluate the effect of the endoscopic activity in the coagulation profile in CD in clinical remission. Methods: Between May/2015 and April/2017, 261 CD patients in supposed clinical remission, were screened, and 229 had a colonoscopy done, resulting in the inclusion of 164 CD patients in clinical remission confirmed by a CDAI <= 150. They were allocated in two groups: 75 in the endoscopic activity (EA) group (SES-CD >= 7), and 89 in the endoscopic remission (ER) group (SES-CD <= 2). 50 healthy controls matched for sex and age were chosen. We measured in the 3 groups, in addition to the generation of thrombin - through the Calibrated Automated Thrombogram (CAT), with and without thrombomodulin, - the activity of tissue factor (TF), fibrinogen, D-dimer, Factor VIII, ADAMTS-13 and von Willebrand Factor - antigen (VWF) and ristocetin cofactor (VWF:RCo). We collected data regarding the duration of the disease, extension, behavior, location, pharmacological treatment, previous history of surgeries, fecal calprotectin, quality of life (through IBDQ), as well as risk factors for TE such as recent hospitalization, current corticoid use, smoking status, as well as markers of hereditary or acquired thrombophilia. We followed the patients for 1 year of observation, evaluating the variation in CDAI and IBDQ. Results: Most of the patients had ileocolonic involvement (43%), with inflammatory behavior (40%), followed by stenosing (30%) and fistulizing (30%). 67% were in use of immunosuppressors and 52% in use of biological drugs. Risk factors for TE besides other markers of thrombophilia, including protein C and S deficiency, anticardiolipin, protein C resistance, antithrombin, prothrombin and Factor V mutations, were similar in both groups except for the lupus anticoagulant, higher in the EA group (8.1% vs. 1.3%, p = 0.047). As expected, the EA group had significantly higher levels of CRP, fecal calprotectin and platelets. In addition, this group had a higher activity of TF vs. ER group vs. controls (127 vs. 103 vs. 84, p = 0.001). Although the DC group had had higher levels of VWF and VWF:RCo, VWF/ADAMTS-13, Factor VIII and thrombomodulin vs. controls, there was no statistical difference between the EA and ER groups. Thrombin generation levels were similar between the 3 groups, with or without thrombomodulin. Conclusion: These data show that there is an inherent endothelial dysfunction in CD, moreover in patients with EA, this dysfunction may be even greater, due to the exposure of TF. Although the presence of inflammation and endothelial damage contribute to this procoagulant condition, in patients with subclinical disease, there is a permanent compensatory state, since the amount of thrombin generated was the same between the groups. This balance may be compromised by other thromboembolic factors, thus increasing the risk of thrombosis

Atividade endoscópica

Coagulação

Coagulation

Crohn's disease

Doença de Crohn

Endoscopic activity

Fator tecidual

Tissue factor

Tromboembolismo venoso

Venous thromboembolism

La maladie veineuse thromboembolique : étude des facteurs de risque de récidive / Venous thromboembolism : risk factors for recurrence

Olié, Valérie

24 May 2011

A partir des données de deux études de cohortes hospitalières françaises (MEVE etFARIVE), nous nous sommes intéressés aux facteurs de risque de récidive de maladieveineuse thromboembolique (MVTE).Nous avons confirmé un excès de risque de récidive de MVTE chez les hommescomparés aux femmes et montré que cette relation dépendait en partie de l’âge, de lamutation du FV Leiden et de la prise d'hormones au premier événement. Une analyse enfonction du sexe a mis en évidence que l’âge, l’obésité et des niveaux élevés de D-dimèresaugmentaient significativement le risque de récidive de MVTE chez les femmes. Par ailleurs,contrairement aux estrogènes oraux, les estrogènes transdermiques seuls ou combinés à laprogestérone micronisée n'exposaient pas les femmes ménopausées à un risque accru derécidive de MVTE. Chez les hommes, la mutation du facteur V Leiden, un antécédent familialde maladie artérielle et un premier événement idiopathique étaient des facteurs de risqueindépendants de récidive.L'identification de profils de risque différents en fonction du sexe pourrait permettreune meilleure stratification du risque de récidive de MVTE. Ces résultats devraientcontribuer à améliorer la prise en charge de la maladie par une évaluation individuelle de ladurée optimale du traitement anticoagulant. De plus, une bonne sécurité d’emploi desestrogènes transdermiques seuls ou combinés à la progestérone micronisée ouvre desperspectives cliniques intéressantes dans le traitement des troubles sévères de laménopause chez des patientes avec un antécédent personnel de MVTE.Mots / Based on data from two French hospital cohort studies, we investigated the riskfactors for recurrent venous thromboembolism (VTE).We confirmed the higher risk of recurrent VTE among men compared with womenand we suggested that this relation depended on age, Factor V Leiden mutation andhormone-related first event. A sex-specific analysis showed that advancing age, obesity andelevated D-dimer significantly increased the risk of recurrent VTE in women. Moreover, oralbut not transdermal estrogens, were associated with a higher risk of recurrent VTE amongpostmenopausal women. In men, factor V Leiden mutation, family history of arterial diseaseand an idiopathic first event were independent risk factors for VTE recurrence.The identification of sex-specific risk factors provides a new insight to riskstratification for VTE recurrence. These results could improve the prevention of this diseaseby an individual assessment of the optimal duration of anticoagulation therapy. In addition,our results provide first evidence supporting the safety of transdermal estrogens alone orcombined with micronized progesterone with respect to VTE recurrence risk. These datacould have important clinical implications for women with personal history of VTE whorequire hormone therapy for severe postmenopausal symptoms.

Maladie veineuse thromboembolique,

Récidive

Facteurs de risque

Sexe

Estrogènes transdermiques

Venous thromboembolism,

Recurrence

Risk factors

Gender

Transdermal estrogens

Direct Thrombin Inhibitors in Treatment and Prevention of Venous Thromboembolism: Dose – Concentration – Response Relationships

Cullberg, Marie

January 2006

<p>For prevention and treatment of thrombotic diseases with an anticoagulant drug it is important that an adequate dose is given to avoid occurrence or recurrence of thrombosis, without increasing the risk of bleeding and other adverse events to unacceptable levels. The aim of this thesis was to develop mathematical models that describe the dose-concentration (pharmacokinetic) and concentration-response (pharmacodynamic) relationships of direct thrombin inhibitors, in order to estimate optimal dosages for treatment and long-term secondary prevention of venous thromboembolism (VTE).</p><p>Population pharmacokinetic-pharmacodynamic models were developed, based on data from clinical investigations in healthy volunteers and patients receiving intravenous inogatran, subcutaneous melagatran and/or its oral prodrug ximelagatran. The benefit-risk profiles of different ximelagatran dosages were estimated using clinical utility functions. These functions were based on the probabilities and fatal consequences of thrombosis, bleeding and elevation of the hepatic enzyme alanine aminotransferase (ALAT).</p><p>The studies demonstrate that the pharmacokinetics of melagatran and ximelagatran were predictable and well correlated to renal function. The coagulation marker, activated partial thromboplastin time (APTT), increased non-linearly with increasing thrombin inhibitor plasma concentration. Overall, the systemic melagatran exposure (AUC) and APTT were similarly predictive of thrombosis and bleedings. The identified relationship between the risk of ALAT-elevation and melagatran AUC suggests that the incidence approaches a maximum at high exposures. The estimated clinical utility was favourable compared to placebo in the overall study population and in special subgroups of patients following fixed dosing of ximelagatran for long-term secondary prevention of VTE. Individualized dosing was predicted to add limited clinical benefit in this indication.</p><p>The models developed can be used to support the studied dosage and for selection of alternative dosing strategies that may improve the clinical outcome of ximelagatran treatment. In addition, the models may be extrapolated to aid the dose selection in clinical trials with other direct thrombin inhibitors.</p>

Pharmaceutical biosciences

Ximelagatran

pharmacokinetic

pharmacodynamic

activated partial thromboplastin time

utility function

dosing strategy

venous thromboembolism

NONMEM

Farmaceutisk biovetenskap

Direct Thrombin Inhibitors in Treatment and Prevention of Venous Thromboembolism: Dose – Concentration – Response Relationships

Cullberg, Marie

January 2006

For prevention and treatment of thrombotic diseases with an anticoagulant drug it is important that an adequate dose is given to avoid occurrence or recurrence of thrombosis, without increasing the risk of bleeding and other adverse events to unacceptable levels. The aim of this thesis was to develop mathematical models that describe the dose-concentration (pharmacokinetic) and concentration-response (pharmacodynamic) relationships of direct thrombin inhibitors, in order to estimate optimal dosages for treatment and long-term secondary prevention of venous thromboembolism (VTE). Population pharmacokinetic-pharmacodynamic models were developed, based on data from clinical investigations in healthy volunteers and patients receiving intravenous inogatran, subcutaneous melagatran and/or its oral prodrug ximelagatran. The benefit-risk profiles of different ximelagatran dosages were estimated using clinical utility functions. These functions were based on the probabilities and fatal consequences of thrombosis, bleeding and elevation of the hepatic enzyme alanine aminotransferase (ALAT). The studies demonstrate that the pharmacokinetics of melagatran and ximelagatran were predictable and well correlated to renal function. The coagulation marker, activated partial thromboplastin time (APTT), increased non-linearly with increasing thrombin inhibitor plasma concentration. Overall, the systemic melagatran exposure (AUC) and APTT were similarly predictive of thrombosis and bleedings. The identified relationship between the risk of ALAT-elevation and melagatran AUC suggests that the incidence approaches a maximum at high exposures. The estimated clinical utility was favourable compared to placebo in the overall study population and in special subgroups of patients following fixed dosing of ximelagatran for long-term secondary prevention of VTE. Individualized dosing was predicted to add limited clinical benefit in this indication. The models developed can be used to support the studied dosage and for selection of alternative dosing strategies that may improve the clinical outcome of ximelagatran treatment. In addition, the models may be extrapolated to aid the dose selection in clinical trials with other direct thrombin inhibitors.

Pharmaceutical biosciences

Ximelagatran

pharmacokinetic

pharmacodynamic

activated partial thromboplastin time

utility function

dosing strategy

venous thromboembolism

NONMEM

Farmaceutisk biovetenskap

Prävalenz schlafbezogener Atemstörungen bei Patienten mit Thrombose und Lungenembolie / Sleep-disordered breathing in patients with deep vein thrombosis and acute pulmonary embolism

Stein, Annika

06 August 2012

No description available.

610 Medizin, Gesundheit

MED 416

Medicine

Obstruktives Schlafapnoesyndrom

Venöse Thromboembolie

Polygraphie

Obstructive sleep apnea

venous thromboembolism

polygraphy

44.84

Vliv vrozených hyperkoagulačních stavů na hladinu D-d se zaměřením na gravidní ženy

ŠTÍCHOVÁ, Zuzana

January 2017

The thesis analyses the female patients' data from Clinical hematology department in České Budějovice hospital from year 2014 to 2015 and tries to statistically confirm connection between D-dimer level and hypercoagulable states described in previous bachelor thesis. D-dimer assay is due to negative predictive value and high sensitivity an initial laboratory test to rule out tromboembolic disease. However, it has low specificity. The elevated level of D-dimer is observed in conditions like infection, trauma, acute cancer, recent surgery or pregnancy and last studies showed increased D-dimer level even in combination with inherited hypercoagulable states. Thus, it is necessary to analyse the level of D-dimer in pregnant women related to specific hypercoagulable states. Moreover, the thesis analyses the influence of other factors like anticoagulation therapy on D-dimer level and tries to find connection between D-dimer level and pregnancy associated complication, birth weight or a type of delivery.

Trombofilie a trombotické komplikace u nemocných se závažnou sepsí. / Thrombophilia and thrombotic complications in severe septic patients

Zenáhlíková, Zuzana

January 2013

Introduction: Thrombotic events are among the most serious complications of sepsis and also the most frequent causes of morbidity and mortality in patients with sepsis. Currently, the administration of low molecular weight heparins (LMWH) is recommended in patients with severe sepsis for prophylaxis of these complications. However, this prophylaxis often fails. Objectives of the study: One of the objectives of our study was to examine changes in haemostasis in relation to the inflammatory response during 15 days of severe sepsis. The next objective was to determine whether a prophylactic inhibition of F Xa in the range from 0.2 to 0.4 IU/mL is achieved in these patients, if they receive the recommended prophylaxis with LMWH. We also recorded the dynamics of changes in the F Xa inhibition during the entire study period. Moreover, we tried to identify the factors that may affect the antithrombotic efficacy of the subcutaneously administered enoxaparin. Patient population and methods: A total of 35 ICU patients meeting the criteria of severe sepsis were enrolled in the study. Only 16 of these patients could be followed throughout the entire 15-day period. Patients were treated according to the current guidelines, including LMWH prophylaxis; enoxaparin (40 mg sc per day) was used in this study....

Avaliação da hemostasia na Doença de Crohn subclínica: papel da atividade endoscópica / Hemostatic parameters in Crohn\'s Disease in clinical remission: role of endoscopic activity

Adriana Ribas Andrade

25 July 2018

Introdução: Pacientes com Doença de Crohn (DC) apresentam alto risco de eventos tromboembólicos (TE), muitas vezes, associados a alta morbimortalidade. É conhecido o papel da inflamação na fisiopatologia da trombose na doença Inflamatória Intestinal (DII), entretanto, o significado da inflamação subclínica ainda se mantém obscuro na literatura. Este estudo avaliou o efeito da atividade endoscópica no perfil de coagulação dos pacientes com DC em remissão clínica. Métodos: entre os dias 22 de maio de 2015 e 26 de abril de 2017, foram triados 261 pacientes com DC em possível remissão clínica, sendo realizadas ao todo 229 colonoscopias. Das 229 colonoscopias realizadas, 164 pacientes estavam realmente em remissão clínica (confirmados com CDAI <= 150) e foram alocados em dois grupos: 75 no grupo de atividade endoscópica (AE) (SES-CD >= 7), 89 no grupo de remissão endoscópica (RE) (SES-CD <= 2). Cinquenta controles saudáveis pareados por sexo e idade foram eleitos. Medimos, nos 3 grupos, além da geração de trombina - pelo método Calibrated Automated Thrombogram (CAT), com e sem trombomodulina, - a atividade do fator tecidual (FT), fibrinogênio, D-dímero, Fator VIII, ADAMTS-13, Fator de von Willebrand - antígeno e cofator de ristocetina (cWF). Coletamos dados sobre a duração da doença, extensão, comportamento, localização, tratamento farmacológico, história prévia de cirurgias, calprotectina fecal, qualidade de vida (por meio do IBDQ), além dos fatores de risco para TE, como hospitalização recente, uso de corticoide atual, status do tabagismo, assim como marcadores de trombofilia hereditária ou adquirida. Seguimos os pacientes por 1 ano de observação, avaliando a variação no CDAI e IBDQ no período. Resultados: A maioria dos pacientes apresentou comprometimento ileocolônico (43%), com comportamento inflamatório (40%), seguido de estenosante (30%) e fistulizante (30%). 67% estavam em uso de imunossupressores e 52% em uso de biológicos. Os fatores de risco para TE e todos os outros marcadores de trombofilia, incluindo deficiência de proteína C e S, anticardiolipina, resistência à proteína C, antitrombina, mutações da protrombina e do Fator V, foram semelhantes em ambos os grupos, exceto pelo anticoagulante lúpico, maior no grupo de AE (8,1% vs. 1,3%, p=0,047). Como esperado, o grupo de AE apresentou níveis significativamente maiores de PCR, calprotectina fecal e plaquetas. Além disso, este grupo apresentou uma maior atividade do fator tecidual vs. o grupo de RE vs. controles (127 vs. 103 vs. 84, p = 0,001). Embora o grupo DC tivesse maiores níveis de FVW:Ag e FVW:RCo, FVW/ADAMTS-13, Fator VIII e trombomodulina vs. controles, não houve diferença estatística entre os grupos de AE e RE. Os níveis de geração de trombina foram semelhantes entre os 3 grupos, com ou sem trombomodulina. Conclusão: Esses dados evidenciam que existe uma disfunção endotelial inerente à DC, e, que, em pacientes com AE, essa disfunção pode ser ainda maior pela maior exposição do FT. Embora, a presença de inflamação e dano endotelial contribuam para esse estado procoagulante, em pacientes com doença subclínica, há um estado de compensação permanente, uma vez que a quantidade de trombina gerada foi a mesma entre os grupos. Este equilíbrio pode estar comprometido diante de outros fatores tromboembólicos, aumentando, assim, o risco de trombose / Background: Crohn\'s disease patients (CD) have a high risk of thromboembolic events (TE), often associated with high morbidity and mortality. Involvement of inflammation in TE is well known, but significance of the sub-clinical inflammation in this process is not the rule. Thus, the aim of this study is to evaluate the effect of the endoscopic activity in the coagulation profile in CD in clinical remission. Methods: Between May/2015 and April/2017, 261 CD patients in supposed clinical remission, were screened, and 229 had a colonoscopy done, resulting in the inclusion of 164 CD patients in clinical remission confirmed by a CDAI <= 150. They were allocated in two groups: 75 in the endoscopic activity (EA) group (SES-CD >= 7), and 89 in the endoscopic remission (ER) group (SES-CD <= 2). 50 healthy controls matched for sex and age were chosen. We measured in the 3 groups, in addition to the generation of thrombin - through the Calibrated Automated Thrombogram (CAT), with and without thrombomodulin, - the activity of tissue factor (TF), fibrinogen, D-dimer, Factor VIII, ADAMTS-13 and von Willebrand Factor - antigen (VWF) and ristocetin cofactor (VWF:RCo). We collected data regarding the duration of the disease, extension, behavior, location, pharmacological treatment, previous history of surgeries, fecal calprotectin, quality of life (through IBDQ), as well as risk factors for TE such as recent hospitalization, current corticoid use, smoking status, as well as markers of hereditary or acquired thrombophilia. We followed the patients for 1 year of observation, evaluating the variation in CDAI and IBDQ. Results: Most of the patients had ileocolonic involvement (43%), with inflammatory behavior (40%), followed by stenosing (30%) and fistulizing (30%). 67% were in use of immunosuppressors and 52% in use of biological drugs. Risk factors for TE besides other markers of thrombophilia, including protein C and S deficiency, anticardiolipin, protein C resistance, antithrombin, prothrombin and Factor V mutations, were similar in both groups except for the lupus anticoagulant, higher in the EA group (8.1% vs. 1.3%, p = 0.047). As expected, the EA group had significantly higher levels of CRP, fecal calprotectin and platelets. In addition, this group had a higher activity of TF vs. ER group vs. controls (127 vs. 103 vs. 84, p = 0.001). Although the DC group had had higher levels of VWF and VWF:RCo, VWF/ADAMTS-13, Factor VIII and thrombomodulin vs. controls, there was no statistical difference between the EA and ER groups. Thrombin generation levels were similar between the 3 groups, with or without thrombomodulin. Conclusion: These data show that there is an inherent endothelial dysfunction in CD, moreover in patients with EA, this dysfunction may be even greater, due to the exposure of TF. Although the presence of inflammation and endothelial damage contribute to this procoagulant condition, in patients with subclinical disease, there is a permanent compensatory state, since the amount of thrombin generated was the same between the groups. This balance may be compromised by other thromboembolic factors, thus increasing the risk of thrombosis

Atividade endoscópica

Coagulação

Doença de Crohn

Fator tecidual

Tromboembolismo venoso

Coagulation

Crohn's disease

Endoscopic activity

Tissue factor

Venous thromboembolism

Chirurgie bariatrique, hypercoagulabilité et maladie thromboembolique veineuse : explorations à partir d'une étude de cohorte locale et d'une étude de cohorte nationale / Bariatric surgery, hypercoagulable state and venous thromboembolism disease : from monocentric study to nationwide cohort study

Thereaux, Jérémie

16 January 2017

Introduction: L’obésité est un facteur connu d’hypercoagulabilité in vitro et in vivo. Cependant peu d’études se sont intéressées aux facteurs de risque d’hypercoagulabilité biologique chez le patient obèse morbide, à sa variation après chirurgie bariatrique (CB) ainsi qu’aux facteurs de risques de maladie thromboembolique veineuse (MTEV) postopératoire après CB. Matériel et Méthodes: Tous les patients destinés à une CB entre le 1er Septembre 2014 et le 31 Janvier 2016 au CHU de Brest étaient éligibles pour notre étude de cohorte locale et ont bénéficié d’un large bilan sanguin préopératoire et à 12 mois postopératoires, incluant des tests de génération de thrombine (GT) avec mesure du potentiel endogène de thrombine (ETP), une méthode validée globale d’évaluation de la coagulation. En parallèle, nous avons extrait de la base du SNIIRAM de l’assurance maladie, tous les patients opérés d’une CB entre le 1er Janvier 2012 et le 30 Septembre 2014 et déterminer la fréquence d’une MTEV dans les 90 jours suivants la CB. Résultats: Cent-deux patients étaient inclus dans notre étude de cohorte brestoise. Les facteurs de risque (OR (95% IC)) de présenter un ETP dans le 4ème quartile de distribution étaient : taux de cholestérol total augmenté (Pas=1mmol/l) (2,6 (1,2-5,4);P =0,01) et taux de fibrinogène augmenté (Pas=1 g/l) (2,2; (1,1-4,5);P = 0,03). A un an post-opératoire (%perte de poids: 33.1±8.3), on retrouvait une baisse significative de l’ETP (%) (111 (96-129) vs. 84 (72-102) ; P<0.001), du taux de fibrinogène (g/l) (4,2±0,8 vs. 3,6±0,8 ; P<0.001) et une baisse non significative du taux de cholestérol total (mmol/l) (4,8±0,8 vs. 4,6±1,0; P=0,08). Apres extraction à partir du SNIIRAM, 110.824 patients étaient inclus. Le taux de MTEV dans les 90 jours était de 0,51%. Les principaux facteurs de risque de MTEV retrouvés en analyse multivariée étaient (P<0.001): un antécédent de MTEV (6,41 (4,50-9,14)), des complications post-opératoires (9,23 (7,30-11,68)), une défaillance cardiaque (2,45 (1,48-4,06), une chirurgie par laparotomie (2,38 (1,59-3,45)), un IMC ≥ 50 kg/m² (1,67 (1,28-2,18)), une sleeve gastrectomy (2,02 (1,39-2,93)) et une procédure de deuxième intention (1,37 (1,10-1,72)). Conclusion : Sur une étude de cohorte de plus de 110.000 patients, nous identifions un taux faible de MTEV dans les 90 jours post-opératoires après CB dépendant de facteurs de risque individuels et liés à la chirurgie. De surcroit nous identifions une baisse de la GT à 1 an post-opératoire en parallèle à une perte de poids massive et à une diminution de l’état inflammatoire. / Introduction: Obese patients are known to be in an in vitro and in an in vivo hypercoagulable state relative to normal-weight patients. Studies focusing exclusively on morbidly obese patients are lacking. Our study aimed to identify markers of enhanced coagulability, to compare its evolution one year after bariatric surgery (BS) and to determine risk factors of venous thromboembolism (VTE) within 90 postoperative days. Methods: All patients scheduled for bariatric surgery (BS) between September 1, 2014 and January 31, 2016 in Brest University Hospital were eligible for our prospective local study. In vitro coagulation was assessed using thrombin generation (TG) tests (Endogenous thrombin potential (ETP)). Data on all patients undergoing BS in France from 1st January 2012 to 30 September 2014 were also extracted from the database of the French national health care (SNIIRAM) to determine the rate of VTE in the 90 days after surgery. Results: One hundred and two patients were included in our study assessing TG. Risk factors for enhanced TG (ETP in the 4th quartile) were increased total cholesterol level (Step=1mmol/l) (2.6 (1.2-5.4); P =0.01) and increased fibrinogen level (Step=1g/l) (2.2 (1.1-4.5); P=0.03). At 12 postoperative months, we found a significant lower ETP (%) (111 (96-129) vs. 84 (72-102 P<0.001)), fibrinogen level (g/l) (4.2±0.8 vs. 3.6±0.8; P<0.001)) and a non-significant trend for lower total cholesterol level (mmol/l) (4.8±0.8 vs. 4.6±1.0; P=0.08). After extraction of the SNIIRAM database, 110,824 patients were included with a rate of VTE of 0.51% (90 post-operative days). Main risk factors for postoperative VTE were (p<0.001): history of VTE (6.41 (4.50-9.14)), postoperative complications (9.23 (7.30-11.68)), heart failure (2.45 (1.48-4.06), open approach (2.38 (1.59-3.45)), BMI ≥ 50 kg/m² (1.67 (1.28-2.18)), sleeve gastrectomy (2.02 (1.39-2.93)) and redo procedure (1.37 (1.10-1.72)). Conclusions: Our study highlights the role of total cholesterol and blood inflammatory marker levels in enhancing TG in morbidly obese patients and shows a decrease of TG at 12 months after BS. The risk of postoperative VTE after BS is low depending on the individual risk level.

Chirurgie bariatrique

Génération thrombine

Maladie thromboembolique veineuse

Hypercoagulabilité

Bariatric surgery

Thrombin generation

Venous thromboembolism

Hypercoagulable state

573.159

617.43

Comparison of Postoperative Bleeding in Total Hip and Knee Arthroplasty Patients Receiving Rivaroxaban, Enoxaparin, or Aspirin for Thromboprophylaxis

Lindquist, Desirae E., Stewart, David W., Brewster, Aaryn, Waldroup, Caitlin, Odle, Brian L., Burchette, Jessica E., El-Bazouni, Hadi

01 November 2018

Background: Guidelines recommend the use of multiple pharmacologic agents and/or mechanical compressive devices for prevention of venous thromboembolism, but preference for any specific agent is no longer given in regard to safety or efficacy. Objective: To compare postoperative bleeding rates in patients receiving enoxaparin, rivaroxaban, or aspirin for thromboprophylaxis after undergoing elective total hip arthroplasty or total knee arthroplasty. Methods: This retrospective cohort analysis evaluated patients who received thromboprophylaxis with either enoxaparin, rivaroxaban, or aspirin. All data were collected from the electronic medical record. The primary outcome was any postoperative bleeding. Results: A total of 1244 patients were included with 366 in the aspirin, 438 in the enoxaparin, and 440 in the rivaroxaban arms. Those who received aspirin or enoxaparin were less likely to experience any bleeding compared to those patients who received rivaroxaban (P <.05). There was also a lower rate of major bleeding in these groups, but the differences were not significant. Conclusions: Aspirin and enoxaparin conferred similar bleeding risks, and both exhibited less bleeding than patients who received rivaroxaban.

aspirin

deep vein thrombosis

enoxaparin

prophylaxis

pulmonary embolism

rivaroxaban

total hip arthroplasty

total knee arthroplasty

venous thromboembolism

Pharmacy Practice