Shinichiro Oguni
Sysmex Corporation
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Publication
Featured researches published by Shinichiro Oguni.
British Journal of Haematology | 2004
Carol Briggs; S. Kunka; Daniel P. Hart; Shinichiro Oguni; Samuel J. Machin
A new automated method to reliably quantify reticulated platelets, expressed as the immature platelet fraction (IPF), has been developed utilizing the XE‐2100 blood cell counter with upgraded software (Sysmex, Kobe, Japan). The IPF is identified by flow cytometry techniques and the use of a nucleic acid specific dye in the reticulocyte/optical platelet channel. The clinical utility of this parameter was established in the laboratory diagnosis of thrombocytopenia due to increased peripheral platelet destruction, particularly autoimmune thrombocytopenic purpura (AITP) and thrombotic thrombocytopenic purpura (TTP). Reproducibility and stability results over 48 h were good. An IPF reference range in healthy individuals was established as 1·1–6·1%, with a mean of 3·4%. Patients in whom platelet destruction might be abnormal, were studied and two of these patients followed serially during the course of treatment. The IPF was raised in several disease states. The most significant increases in IPF values were found in patients with AITP (mean 22·3%, range 9·2–33·1%) and acute TTP (mean 17·2%, range 11·2–30·9%). Following patients during treatment demonstrated that as the platelet count recovered the IPF% fell. These results show that a rapid, inexpensive automated method for measuring the IPF% is feasible and should become a standard parameter in evaluating the thrombocytopenic patient.
Clinical and Applied Thrombosis-Hemostasis | 2005
Miho Sakakura; Hideo Wada; Yasunori Abe; Junji Nishioka; Hiroaki Tomatsu; Yukio Hamaguchi; Shinichiro Oguni; Hiroshi Shiku; Tsutomu Nobori
Reticulated platelets (RP) and large platelets (LP) were measured by an automated hematology analyzer (modified R-2000) in 287 healthy volunteers and 131 patients with thrombocytopenia or thrombocytosis. RP was significantly higher in patients with idiopathic thrombocytopenic purpura (ITP), especially in active phase, while RP was markedly lower in patients with essential thrombocytosis (ET) or chronic myelocytic leukemia (CML). LP was significantly higher in patients with ITP, especially in active phase, while LP was markedly lower in patients with aplastic anemia (AA), ET, or CML. In ITP, RP and LP were significantly higher in patients positive for anti-glycoprotein (Gp) IIb/IIIa antibody. RP and LP were poorly correlated with platelet-associated IgG (PAIgG). RP and LP were poorly correlated with plasma thrombopoietin levels, and negatively correlated with platelet count. These results show that RP reflects the pathology of thrombocytopenic disorders, and that measurement of RP is useful for the differential diagnosis and analysis of platelet kinetics.
Clinical and Applied Thrombosis-Hemostasis | 2005
Yasunori Abe; Hideo Wada; Miho Sakakura; Junji Nishioka; Hiroaki Tomatsu; Yukio Hamaguchi; Shinichiro Oguni; Hiroshi Shiku; Tsutomu Nobori
Reticulated platelets (RP) were measured with an automated hematology analyzer (modified R-2000) in 287 healthy volunteers and in 212 patients with thrombocytopenia. In healthy volunteers, the RP was 0.48 ± 0.26% in men and 0.48 ± 0.32% in women. No significant difference in the RP values due to gender or age (21-60 years) was observed. Furthermore, the reverse correlation was observed between platelet counts and RP. The RP was high in patients with idiopathic thrombocytopenic purpura (ITP), those with high fibrinogen and fibrin degradation products (FDP), and those with high C-reactive protein (CRP), but low in patients after chemotherapy. The RP was highest in active phase of ITP, and relatively high in the partial remission phase of aplastic anemia. In patients after chemotherapy, the patients had a minimum phase of RP and then a maximum phase of RP before platelet counts increased. RP was significantly high in the maximum phase and significantly low in the minimum phase. The relationships between platelet count and RP were negatively correlated in patients with ITP, high FDP, or high CRP, but were not correlated in patients with aplastic anemia, liver disease, or after chemotherapy. These results show that RP reflects the pathology of thrombocytopenic disorders and the measurement of RP is useful for the differential diagnoses and analysis of platelet kinetics.
International Journal of Nephrology | 2012
Aya Eguchi; Takahiro Mochizuki; Misao Tsukada; Koji Kataoka; Yukio Hamaguchi; Shinichiro Oguni; Kosaku Nitta; Ken Tsuchiya
Hepcidin is the key mediator of renal anemia, and reliable measurement of serum hepcidin levels has been made possible by the ProteinChip system. We therefore investigated the iron status and serum hepcidin levels of peritoneal dialysis (PD) patients who had not received frequent doses of an erythrocytosis-stimulating agent (ESA) and had not received iron therapy. In addition to the usual iron parameters, the iron status of erythrocytes can be determined by measuring reticulocyte hemoglobin (RET-He). The mean serum hepcidin level of the PD patients (n = 52) was 80.7 ng/mL. Their serum hepcidin levels were significantly positively correlated with their serum ferritin levels and transferrin saturation (TSAT) levels, but no correlations were found between their serum hepcidin levels and RET-He levels, thereby suggesting that hepcidin has no effect on the iron dynamics of reticulocytes. Since low serum levels of CRP and IL-6, biomarkers of inflammation, were not correlated with the serum hepcidin levels, there is likely to be a threshold for induction of hepcidin expression by inflammation.
Thrombosis Research | 2006
Yasunori Abe; Hideo Wada; Hiroaki Tomatsu; Akane Sakaguchi; Junji Nishioka; Yasunori Yabu; Katsuya Onishi; Kaname Nakatani; Yoshitaka Morishita; Shinichiro Oguni; Tsutomu Nobori
Transfusion Medicine | 2006
Carol Briggs; Daniel P. Hart; S. Kunka; Shinichiro Oguni; Samuel J. Machin
Archive | 1998
Tomohiro Tsuji; Takashi Sakata; Yoshiro Ikeuchi; Shinichiro Oguni
Archive | 2007
Tomohiro Tsuji; Ayumu Yoshida; Shinichiro Oguni
Archive | 2004
Shinichiro Oguni; Seido Biwa
Archive | 2007
Tomohiro Tsuji; Ayumu Yoshida; Shinichiro Oguni