Direct Oral Anticoagulants Form Thrombus Different From Warfarin in a Microchip Flow Chamber System

Abstract Direct oral anticoagulants (DOACs) have low risk of intracranial hemorrhage compared to warfarin. We sought to clarify the different mechanisms responsible for suppression of bleeding events using the Total Thrombus-formation Analysis System (T-TAS), a flow-microchip chamber with thrombogen...

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Main Authors: Masanobu Ishii, Koichi Kaikita, Miwa Ito, Daisuke Sueta, Yuichiro Arima, Seiji Takashio, Yasuhiro Izumiya, Eiichiro Yamamoto, Megumi Yamamuro, Sunao Kojima, Seiji Hokimoto, Hiroshige Yamabe, Hisao Ogawa, Kenichi Tsujita
Format: Article
Language:English
Published: Nature Publishing Group 2017-08-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-017-07939-6
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spelling doaj-a051c3d32ddf4095a83804444ee2443f2020-12-08T03:12:54ZengNature Publishing GroupScientific Reports2045-23222017-08-01711910.1038/s41598-017-07939-6Direct Oral Anticoagulants Form Thrombus Different From Warfarin in a Microchip Flow Chamber SystemMasanobu Ishii0Koichi Kaikita1Miwa Ito2Daisuke Sueta3Yuichiro Arima4Seiji Takashio5Yasuhiro Izumiya6Eiichiro Yamamoto7Megumi Yamamuro8Sunao Kojima9Seiji Hokimoto10Hiroshige Yamabe11Hisao Ogawa12Kenichi Tsujita13Department of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesDepartment of Cardiovascular Medicine, National Cerebral and Cardiovascular CenterDepartment of Cardiovascular Medicine, Kumamoto University Graduate School of Medical SciencesAbstract Direct oral anticoagulants (DOACs) have low risk of intracranial hemorrhage compared to warfarin. We sought to clarify the different mechanisms responsible for suppression of bleeding events using the Total Thrombus-formation Analysis System (T-TAS), a flow-microchip chamber with thrombogenic surfaces. Blood samples were obtained at Off- and On-anticoagulant (trough) from 120 consecutive patients with atrial fibrillation (warfarin; n = 29, dabigatran; n = 19, rivaroxaban; n = 47, apixaban; n = 25), which were used for T-TAS to compute the area under the curve (AUC) (AR10-AUC30) in the AR chip, and to measure plasma concentrations of DOACs at On-anticoagulant. In addition, the two-dimensional area covered by thrombi (%) in the capillary was analyzed every 3 minutes after sample applications. The AR10-AUC30 correlated weakly and negatively with plasma concentrations of DOACs, and the levels at On-anticoagulant were lower in all groups than at Off-anticoagulant. AR10-AUC30 levels at Off- and On-anticoagulant were identical among the groups. The thrombi areas in early phase were significantly larger in rivaroxaban and apixaban than warfarin and dabigatran groups. The findings suggested that visual analysis of the AR-chip can identify the differential inhibitory patterns of warfarin and DOACs on thrombus formation under flow condition.https://doi.org/10.1038/s41598-017-07939-6
collection DOAJ
language English
format Article
sources DOAJ
author Masanobu Ishii
Koichi Kaikita
Miwa Ito
Daisuke Sueta
Yuichiro Arima
Seiji Takashio
Yasuhiro Izumiya
Eiichiro Yamamoto
Megumi Yamamuro
Sunao Kojima
Seiji Hokimoto
Hiroshige Yamabe
Hisao Ogawa
Kenichi Tsujita
spellingShingle Masanobu Ishii
Koichi Kaikita
Miwa Ito
Daisuke Sueta
Yuichiro Arima
Seiji Takashio
Yasuhiro Izumiya
Eiichiro Yamamoto
Megumi Yamamuro
Sunao Kojima
Seiji Hokimoto
Hiroshige Yamabe
Hisao Ogawa
Kenichi Tsujita
Direct Oral Anticoagulants Form Thrombus Different From Warfarin in a Microchip Flow Chamber System
Scientific Reports
author_facet Masanobu Ishii
Koichi Kaikita
Miwa Ito
Daisuke Sueta
Yuichiro Arima
Seiji Takashio
Yasuhiro Izumiya
Eiichiro Yamamoto
Megumi Yamamuro
Sunao Kojima
Seiji Hokimoto
Hiroshige Yamabe
Hisao Ogawa
Kenichi Tsujita
author_sort Masanobu Ishii
title Direct Oral Anticoagulants Form Thrombus Different From Warfarin in a Microchip Flow Chamber System
title_short Direct Oral Anticoagulants Form Thrombus Different From Warfarin in a Microchip Flow Chamber System
title_full Direct Oral Anticoagulants Form Thrombus Different From Warfarin in a Microchip Flow Chamber System
title_fullStr Direct Oral Anticoagulants Form Thrombus Different From Warfarin in a Microchip Flow Chamber System
title_full_unstemmed Direct Oral Anticoagulants Form Thrombus Different From Warfarin in a Microchip Flow Chamber System
title_sort direct oral anticoagulants form thrombus different from warfarin in a microchip flow chamber system
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2017-08-01
description Abstract Direct oral anticoagulants (DOACs) have low risk of intracranial hemorrhage compared to warfarin. We sought to clarify the different mechanisms responsible for suppression of bleeding events using the Total Thrombus-formation Analysis System (T-TAS), a flow-microchip chamber with thrombogenic surfaces. Blood samples were obtained at Off- and On-anticoagulant (trough) from 120 consecutive patients with atrial fibrillation (warfarin; n = 29, dabigatran; n = 19, rivaroxaban; n = 47, apixaban; n = 25), which were used for T-TAS to compute the area under the curve (AUC) (AR10-AUC30) in the AR chip, and to measure plasma concentrations of DOACs at On-anticoagulant. In addition, the two-dimensional area covered by thrombi (%) in the capillary was analyzed every 3 minutes after sample applications. The AR10-AUC30 correlated weakly and negatively with plasma concentrations of DOACs, and the levels at On-anticoagulant were lower in all groups than at Off-anticoagulant. AR10-AUC30 levels at Off- and On-anticoagulant were identical among the groups. The thrombi areas in early phase were significantly larger in rivaroxaban and apixaban than warfarin and dabigatran groups. The findings suggested that visual analysis of the AR-chip can identify the differential inhibitory patterns of warfarin and DOACs on thrombus formation under flow condition.
url https://doi.org/10.1038/s41598-017-07939-6
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