Kenzo Machida
Sony Broadcast & Professional Research Laboratories
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Featured researches published by Kenzo Machida.
Analytical Chemistry | 2015
Yoshihito Hayashi; Marc-Aurele Brun; Kenzo Machida; Masayuki Nagasawa
Dielectric blood coagulometry (DBCM) is intended to support hemostasis management by providing comprehensive information on blood coagulation from automated, time-dependent measurements of whole blood dielectric spectra. We discuss the relationship between the series of blood coagulation reactions, especially the aggregation and deformation of erythrocytes, and the dielectric response with the help of clot structure electron microscope observations. Dielectric response to the spontaneous coagulation after recalcification presented three distinct phases that correspond to (P1) rouleau formation before the onset of clotting, (P2) erythrocyte aggregation and reconstitution of aggregates accompanying early fibrin formation, and (P3) erythrocyte shape transformation and/or structure changes within aggregates after the stable fibrin network is formed and platelet contraction occurs. Disappearance of the second phase was observed upon addition of tissue factor and ellagic acid for activation of extrinsic and intrinsic pathways, respectively, which is attributable to accelerated thrombin generation. A series of control experiments revealed that the amplitude and/or quickness of dielectric response reflect platelet function, fibrin polymerization, fibrinolysis activity, and heparin activity. Therefore, DBCM sensitively measures blood coagulation via erythrocytes aggregation and shape changes and their impact on the dielectric permittivity, making possible the development of the battery of assays needed for comprehensive coagulation testing.
Biorheology | 2017
Yoshihito Hayashi; Marc-Aurele Brun; Kenzo Machida; Seungmin Lee; Aya Murata; Shinji Omori; Hidetoshi Uchiyama; Yoshinori Inoue; Toshifumi Kudo; Takahiro Toyofuku; Masayuki Nagasawa; Isao Uchimura; Tomomasa Nakamura
Background: In a whole blood coagulation test, the concentration of any in vitro diagnostic agent in plasma is dependent on the hematocrit level but its impact on the test result is unknown. Objective: The aim of this work was to clarify the effects of reagent concentration, particularly Ca2+, and to find a method for hematocrit estimation compatible with the coagulation test. Methods: Whole blood coagulation tests by dielectric blood coagulometry (DBCM) and rotational thromboelastometry were performed with various concentrations of Ca2+ or on samples with different hematocrit levels. DBCM data from a previous clinical study of patients who underwent total knee arthroplasty were re-analyzed. Results: Clear Ca2+ concentration and hematocrit level dependences of the characteristic times of blood coagulation were observed. Rouleau formation made hematocrit estimation difficult in DBCM, but use of permittivity at around 3 MHz made it possible. The re-analyzed clinical data showed a good correlation between permittivity at 3 MHz and hematocrit level (R2=0.83). Conclusions: Changes in the hematocrit level may affect whole blood coagulation tests. DBCM has the potential to overcome this effect with some automated correction using results from simultaneous evaluations of the hematocrit level and blood coagulability.
Archive | 2008
Mari Ichimura; Noriyuki Kishii; Kenzo Machida; 典之 岸井; 真理 市村; 賢三 町田
Archive | 2012
Noriyuki Kishii; Mari Ichimura; Kenzo Machida
Archive | 2009
Kenzo Machida; Noriyuki Kishii; Mari Ichimura; Masanobu Tanaka
Archive | 2009
Mari Ichimura; Noriyuki Kishii; Kenzo Machida; Masanobu Tanaka
Archive | 2017
Yoshihito Hayashi; Marcaurele Brun; Kenzo Machida
Archive | 2014
Tomohiko Nakamura; Kenzo Machida
Archive | 2010
Kenzo Machida; Noriyuki Kishii; Mari Ichimura; Kazumine Ito; Takuya Kishimoto; Naohisa Sakamoto
Archive | 2009
Mari Ichimura; Kenzo Machida; Noriyuki Kishii; Masanobu Tanaka