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Dive into the research topics where Kobayashi I is active.

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Featured researches published by Kobayashi I.


Stroke | 1983

Platelet function tests in thrombotic cerebrovascular disorders.

Shinichiro Uchiyama; M Takeuchi; M Osawa; Kobayashi I; Shoichi Maruyama; M Aosaki; K Hirosawa

A variety of platelet function tests were performed in patients with four forms of obstructive cerebrovascular disease (CVD); transient ischemic attacks (TIA), reversible ischemic neurological deficit (RIND), cerebral infarct, and cerebral embolism of cardiac source in rheumatic valvular heart disease (RVHD). Platelet studies included platelet aggregation induced by ADP and ristocetin, spontaneous platelet aggregation, von Willebrand factor (VIII:vWF), platelet aggregation enhancing factor (PAEF), and percentage of large platelets (megathrombocytes). Serial testing was carried out in acute stroke patients. The effect of aspirin therapy was also evaluated. A clear difference in results was observed between patients with cardiogenic embolism and those with other forms of CVD. In patients with TIA, RIND, and cerebral infarct, platelet aggregation, both induced and spontaneous, was enhanced along with elevation of plasma VIII:vWF and PAEF, and increased percentage of megathrombocytes. In patients with cardiogenic embolism, however, these studies were negative except for percent megathrombocytes. This value was increased in the embolic patients with RVHD in comparison with non-embolic patients with RVHD. Increase in platelet aggregation to ADP and percent megathrombocytes developed slowly over a week following stroke. Induced and spontaneous platelet aggregation, and percent megathrombocytes could be normalized with 600 mg aspirin p.o. These studies suggest that a systemic increase of hyperaggregable platelets and of plasma activators of platelet function exists in thrombotic CVD and may be related to its pathogenesis, while local hemodynamic factors may be more important in the thrombogenesis of cardiogenic embolism.


Stroke | 1989

Combination therapy with low-dose aspirin and ticlopidine in cerebral ischemia.

Shinichiro Uchiyama; Reiko Sone; Takashi Nagayama; Yasuro Shibagaki; Kobayashi I; Shoichi Maruyama; Kiyoko Kusakabe

We compared combination therapy with low-dose aspirin plus ticlopidine to therapy with aspirin alone or ticlopidine alone in patients suffering transient ischemic attack or cerebral infarction. In 17, 24, and 23 patients, respectively, 300 mg/day aspirin, 200 mg/day ticlopidine, and 81 mg/day aspirin plus 100 mg/day ticlopidine were administered orally. Aspirin alone markedly inhibited platelet aggregation induced by arachidonic acid, partially inhibited platelet aggregation induced by adenosine diphosphate, and did not inhibit platelet aggregation induced by platelet activating factor. Ticlopidine alone inhibited platelet aggregation induced by adenosine diphosphate and platelet activating factor, but did not inhibit platelet aggregation induced by arachidonic acid. Combination therapy with aspirin plus ticlopidine markedly inhibited platelet aggregation induced by all three agonists. Plasma concentrations of beta-thromboglobulin and platelet factor 4 remained unchanged by aspirin alone, were slightly reduced by ticlopidine alone, and were markedly reduced by aspirin plus ticlopidine. Plasma concentration of thromboxane B2 was reduced by aspirin alone or with ticlopidine, but not by ticlopidine alone. The level of 6-ketoprostaglandin F1 alpha was reduced only by aspirin alone. Bleeding time was significantly prolonged by aspirin alone and by ticlopidine alone, although the greatest prolongation was produced by aspirin plus ticlopidine. Our results indicate that the combination of aspirin plus ticlopidine is a potent antiplatelet strategy, although the clinical importance of the changes observed need to be determined by a properly designed and controlled prospective study.


Psychiatry and Clinical Neurosciences | 1985

L‐Dopa‐Induced Asterixis

Kobayashi I; Mikio Osawa; Kohei Ohta; Shoichi Maruyama

Abstract: Three cases with the occurrence of asterixis during the administration of L‐dopa were reported. Liver and metabolic functions were normal in all the patients. Upon the appearance of asterixis no other involuntary movements probably resulting from an excess administration of L‐dopa were observed. Asterixis occurred accompanied by clinical symptoms such as hallucination and a mild clouding of consciousness by insomnia. Because of its reversal with drug withdrawal, asterixis seemed to be L‐dopa‐related. The biochemical basis of asterixis is not known but may involve the dopaminergic or serotonergic system.


Blood | 1971

Acid Mucopolysaccharides As Cofactor in Formation of Platelet-clumping Substance

Hiroshi Murase; Hagano Ijiri; Tatsuo Shimamoto; Kobayashi I; Takio Shimamoto; Hiroh Yamazaki


Nō to shinkei Brain and nerve | 1990

[A case of inorganic germanium poisoning with peripheral and cranial neuropathy, myopathy and autonomic dysfunction].

Iijima M; Mugishima M; Takeuchi M; Shinichiro Uchiyama; Kobayashi I; Shoichi Maruyama


Nō to shinkei Brain and nerve | 1990

[A case of delayed radiation lumbo-sacral plexopathy].

Numata K; Ito M; Shinichiro Uchiyama; Kobayashi I; Takemiya T; Shoichi Maruyama


Nō to shinkei Brain and nerve | 1991

An autopsy case of progressive supranuclear palsy with olivary hypertrophy

Takeuchi M; Sasaki S; Ito A; Mikio Osawa; Kobayashi I; Shoichi Maruyama


Rinshō shinkeigaku Clinical neurology | 1990

A case of membranous lipodystrophy (Nasu) with diffuse cerebral white matter involvement and cerebellar atrophy on brain CT and MRI

Koichi Shibata; Shinichiro Uchiyama; Megumi Takeuchi; Kobayashi I; Shoichi Maruyama


Rinshō shinkeigaku Clinical neurology | 1991

[A case of Behçet's disease associated with myopathy during cyclosporin treatment].

Koichi Shibata; Megumi Takeuchi; Kikuchi M; Kobayashi I; Shoichi Maruyama


Nō to shinkei Brain and nerve | 1989

Basilar artery migraine associated with transient global amnesia

Yamane K; Hashimoto S; Kobayashi I; Shoichi Maruyama

Collaboration


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Shinichiro Uchiyama

International University of Health and Welfare

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Hiroh Yamazaki

Tokyo Medical and Dental University

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Kohei Ota

Tokyo University of Science

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Shoichi Sasaki

Montefiore Medical Center

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Eiko Kuniyasu

Tokyo Medical and Dental University

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Fujie Numano

Tokyo Medical and Dental University

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Hagano Ijiri

Tokyo Medical and Dental University

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Hiroshi Murase

Tokyo Medical and Dental University

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Mitsuhiko Hirano

Tokyo Medical and Dental University

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Tadahiro Sano

Tokyo Medical and Dental University

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