The quality of the reversion of these serious hemorrhagic accidents under oral anticoagulants depends on the adequate use of reversion products but also on the speed of obtaining hemostasis data allowing to evaluate the effectiveness of this "chemical" hemostasis. . Clot formation can be studied using different visco-elastic methodologies (thromboelastography or thromboelastometry) with a detectable change in clot formation with oral anticoagulants. These techniques have been proven in patients who are often unstable and present with severe trauma with hemorrhagic shock, thus making it possible to guide the transfusion protocol. However, the level of recommendations in these patients, who are often polyhydrated and poly-transfused, is grade 1c due to small-scale studies with difficulty in analyzing the values of the visco-elasticity parameters in these patients. In addition, these methods are little used in current practice because of their difficult reading. The use of visco-elastic methods in patients on oral anticoagulants has been little studied. However, taking an oral anticoagulant mainly causes coagulation disorders. The use of these methods would make it possible to assess the impact of the anticoagulant on hemostasis and to verify the correct reversion of hemostasis parameters. Quantra®, one of the visco-elastic methods, would make it possible to speed up the evaluation in the context of biology relocated to the patient's bed with a simplified reading of the factors involved in the formation of the clot in order to allow an immediate evaluation the quality of the reversion performed which may have an impact on the re-administration of reversion products or even an adaptation of the dose of reversion products according to the initial parameters at the time of severe bleeding before reversion. The objective of this pilot study is to study the metrological evolution, before and after reversion, of the hemostasis parameters evaluated by the Quantra® system from HemoSonics in a patient being his own control in the context of a severe hemorrhage occurring on oral anticoagulants (VKA or DOA).
This multicenter, prospective, cohort pilot study of physiopathology and physio-pharmacology, testing the added value of innovative functional exploration in addition to routine monitoring, in patients eligible for urgent reversion from anticoagulant therapy. This study is part of the patient's routine care without modifying his management. In fact, eligible patients with severe bleeding under oral anticoagulant therapy will be treated according to departmental habits. The study will only consist of the addition of the analysis of a blood sample using the Quantra® before and after reversion without modification of the management. All patients will be followed for the duration of hospitalization. Primary objective : The objective of this pilot study is to study the behavior of viscoelastic hemostasis parameters assessed by the Quantra® System in the context of severe bleeding occurring under oral anticoagulants (VKA or DOA). Secondary objectives : To study the effect of reversion of oral anticoagulants on hemostasis parameters assessed by the Quantra® system in the context of severe bleeding. To study, in the context of severe bleeding, the relationship between the hemostasis parameters assessed by the Quantra® system and: * conventional hemostasis parameters, * the severity of the bleeding events before reversion, in the context of severe bleeding, * recurrent bleeding or thrombotic events occurring during hospitalization. The primary endpoint will be all of the Quantra® parameter values measured during the patient's therapeutic monitoring (before and after) without prioritization. The parameters of Quantra® are: * CT: Clotting time (in seconds) * CTH: Clotting time with Heparinase (in seconds) * CTR: CT / CTH ratio clotting time * CS: overall stiffness of the clot (hPa) * PCS: Contribution of platelets to clot stiffness (hPa) FCS: Contribution of fibrinogen to clot stiffness (hPa) Secondary endpoints: * Classic coagulation tests: (TP / INR), TCA, Fibrinogen, FII, FV, FVII, FX * Drug concentration (for DOA) by dilute thrombin time or specific anti-Xa activity * Type and volume of filling solutes before reversion * Assessment of blood loss (Hb, size of the hematoma) * Clinical outcome of reversion: haemostatic efficacy rate at 24 hours, occurrence of haemorrhagic or thrombotic recurrences during hospitalization * Duration of hospitalization
Study Type
INTERVENTIONAL
Allocation
NA
Purpose
HEALTH_SERVICES_RESEARCH
Masking
NONE
Enrollment
80
one additional tube will be collected during the usual blood test at two different time and analyzed by Quantra ®
University Hospital
Clermont-Ferrand, France
Grenoble University Hospital
Grenoble, France
Edouard Herriot University Hospital
Lyon, France
La Pitié-Salpétrière
Paris, France
Saint Etienne University Hospital
Saint-Etienne, France
Tours University Hospital
Tours, France
change in viscoelastic hemostasis parameters assessed by the Quantra® system in the context of severe bleeding occurring under oral anticoagulants (VKA or DOA)
Quantra® parameters were measured during the patient's therapeutic monitoring (before and after) without prioritization. The parameters of Quantra® are: CT / CTH ratio clotting time overall stiffness of the clot (hPa) Contribution of platelets to clot stiffness (hPa) Contribution of fibrinogen to clot stiffness (hPa)
Time frame: Hour 0 and Hour 0+30min
Change in viscoelastic hemostasis parameters assessed by the Quantra® system in the context of severe bleeding occurring under oral anticoagulants (VKA or DOA)
Quantra® parameters were measured during the patient's therapeutic monitoring (before and after) without prioritization. The parameters of Quantra® are: CT : clotting time (in seconds) CTH clotting time with heparinase (in seconds)
Time frame: Hour 0 and Hour 0+30min
Coagulation test
change in activated partial thromboplastin time (APTT) measures
Time frame: Hour 0; Hour 0+30min; Hour 0+6 hours
Coagulation test
change in prothrombin time test values
Time frame: Hour 0; Hour 0+30min; Hour 0+6 hours
Coagulation test
changes in levels of fibrinogen
Time frame: Hour 0; Hour 0+30min; Hour 0+6 hours
Coagulation test
change in Factor II assay
Time frame: Hour 0; Hour 0+30min; Hour 0+6 hours
Coagulation test
change in Factor V assay
Time frame: Hour 0; Hour 0+30min; Hour 0+6 hours
Coagulation test
change in Factor VII assay
Time frame: Hour 0; Hour 0+30min; Hour 0+6 hours
Coagulation test
change in Factor X assay
Time frame: Hour 0; Hour 0+30min; Hour 0+6 hours
anti-factor Xa activity measurement
change in anti-factor Xa activity measurement
Time frame: Hour 0; Hour 0+30min; Hour 0+6 hours
Type of filling solutes before reversion
Type of filling solutes before reversion
Time frame: Hour 0
Volume of filling solutes before reversion
Volume of filling solutes before reversion
Time frame: Hour 0
Evaluation of blood loss
haemoglobin concentration
Time frame: Hour 0
Evaluation of blood loss
haematoma size
Time frame: Hour 0
Clinical haemostasis evolution
haematoma volume
Time frame: Hour 0+24
Clinical haemostasis evolution
Haematoma pain on numeric scale (0-10 points)
Time frame: Hour 0+24
Clinical issue of reversion
efficacy haemostatic rate at 24 hours
Time frame: Hour 0+24
Clinical issue of reversion
Recurrence of bleeding during hospitalization
Time frame: Hour 0+24
Duration of hospitalization
how many days the patient is hospitalized
Time frame: at the end of hospitalization
phone call
report of any adverse event occured in the month after the end of hospitalization
Time frame: Month 0+1
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