Author: Blasi, Annabel; von Meijenfeldt, Fien A.; Adelmeijer, Jelle; Calvo, Andrea; Ibañez, Cristina; Perdomo, Juan; Carlos Reverter, Juan; Lisman, Ton
Title: In vitro hypercoagulability and ongoing in vivo activation of coagulation and fibrinolysis in COVIDâ€19 patients on anticoagulation Cord-id: 64jxtg9y Document date: 2020_8_6
ID: 64jxtg9y
Snippet: BACKGROUND: COVIDâ€19 is associated with a substantial risk of venous thrombotic events, even in the presence of adequate thromboprophylactic therapy. OBJECTIVES: We aimed to better characterize the hypercoagulable state of COVIDâ€19 patients in patients receiving anticoagulant therapy. METHODS: We took plasma samples of 23 patients with COVIDâ€19 who were on prophylactic or intensified anticoagulant therapy. Twenty healthy volunteers were included to establish reference ranges. RESULTS: COVI
Document: BACKGROUND: COVIDâ€19 is associated with a substantial risk of venous thrombotic events, even in the presence of adequate thromboprophylactic therapy. OBJECTIVES: We aimed to better characterize the hypercoagulable state of COVIDâ€19 patients in patients receiving anticoagulant therapy. METHODS: We took plasma samples of 23 patients with COVIDâ€19 who were on prophylactic or intensified anticoagulant therapy. Twenty healthy volunteers were included to establish reference ranges. RESULTS: COVIDâ€19 patients had a mildly prolonged prothrombin time, high VWF levels and low ADAMTS13 activity. Most rotational thromboelastometry parameters were normal, with a hypercoagulable maximum clot firmness in part of the patients. Despite detectable antiâ€Xa activity in the majority of patients, ex vivo thrombin generation was normal, and in vivo thrombin generation elevated as evidenced by elevated levels of thrombinâ€antithrombin complexes and Dâ€dimers. Plasma levels of activated factor VII were lower in patients, and levels of the platelet activation marker soluble CD40 ligand were similar in patients and controls. Plasminâ€antiplasmin complex levels were also increased in patients despite an in vitro hypofibrinolytic profile. CONCLUSIONS: COVIDâ€19 patients are characterized by normal in vitro thrombin generation and enhanced clot formation and decreased fibrinolytic potential despite the presence of heparin in the sample. Anticoagulated COVIDâ€19 patients have persistent in vivo activation of coagulation and fibrinolysis, but no evidence of excessive platelet activation. Ongoing activation of coagulation despite normal to intensified anticoagulant therapy indicates studies on alternative antithrombotic strategies are urgently required.
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