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Featured researches published by Ryohei Miyake.


Biochemical and Biophysical Research Communications | 1990

Lysophosphatidylcholine: essential role in the inhibition of endothelium-dependent vasorelaxation by oxidized low density lipoprotein.

Mitsuhiro Yokoyama; Ken-ichi Hirata; Ryohei Miyake; Hozuka Akita; Yuichi Ishikawa; Hisashi Fukuzaki

Endothelial cells are known to play an important role in the regulation of vascular tone. Here we demonstrate that modified low density lipoprotein (LDL) with copper oxidation or phospholipase A2 treatment elicits a potent inhibitory action on endothelium-dependent relaxations evoked by acetylcholine, although native LDL does not affect endothelium-dependent relaxations. Phosphatidylcholine of native LDL is converted to lysophosphatidylcholine during these modifications. Furthermore, lysophosphatidylcholine fraction separated from oxidized LDL (0.5mg.protein/ml) by thin layer chromatography abolished endothelium-dependent relaxations, although the remaining lipid fraction had little effects on endothelium-dependent relaxations. These results indicate that lysophosphatidylcholine is the principal substance for the impairment of endothelium-dependent relaxations by oxidized LDL and phospholipase A2 treated LDL.


Biochemical and Biophysical Research Communications | 1984

Activation of calcium-activated, phospholipid-dependent protein kinase (protein kinase C) by new classes of tumor promoters: Teleocidin and debromoaplysiatoxin

Hirota Fujiki; Yasushi Tanaka; Ryohei Miyake; Ushio Kikkawa; Yasutomi Nishizuka; Takashi Sugimura

The new potent tumor promoters teleocidin and debromoaplysiatoxin , which are structurally unrelated to phorbol esters, activate Ca2+-activated, phospholipid-dependent protein kinase (protein kinase C). The concentrations of 12-O-tetradecanoylphorbol-13-acetate, teleocidin and debromoaplysiatoxin for half-maximum activation of protein kinase C were found to be approximately 3 ng/ml, 40 ng/ml and 400 ng/ml, respectively. These three types of tumor promoters bind to protein kinase C, and appear to exhibit their pleiotropic actions through activation of this enzyme.


Biochemical and Biophysical Research Communications | 1984

Activation of protein kinase C by non-phorbol tumor promoter, mezerein

Ryohei Miyake; Yasushi Tanaka; Terutaka Tsuda; Kozo Kaibuchi; Ushio Kikkawa; Yasutomi Nishizuka

Mezerein, classified as a second-stage tumor promoter, has no diacylglycerol-like structure in its molecule, but can activate protein kinase C both in vitro and in vivo. This non-phorbol diterpene competitively inhibits the specific binding of a radioactive tumor-promoting phorbol ester to the enzyme. It is suggestive that tumor-promoting phorbol esters and mezerein cause analogous changes in the membrane to activate protein kinase C, and utilize this protein kinase as a common receptive protein for tumor promotion.


Biochemical and Biophysical Research Communications | 1990

Inhibition of lysophospholipase by cholesterol in rabbit aorta

Ryohei Miyake; Mitsuhiro Yokoyama; Hisashi Fukuzaki

Lysophospholipase activity was measured in rabbit aorta using 1-[1-14C]palmitoyl-sn-glycero-3-phosphocholine as a substrate. The enzyme did not require Ca2+ for its activation and the maximal activation was attained in the presence of EGTA. Cholesterol dose-dependently inhibited the lysophospholipase activity in the soluble fraction and IC50 value was approximately 15 microM. Lineweaver-Burk plot revealed that cholesterol competitively inhibited lysophospholipase and Km values in the presence and absence of cholesterol (15.5 microM) were 12.3 and 2.8 microM, respectively. Vmax values were approximately 475 pmol/min.mg. The results suggest that cholesterol can interact with the enzyme per se, resulting in the inhibition of the lysophospholipase activity in rabbit aorta.


Journal of Biochemistry | 1986

Rapid Assay of Binding of Tumor-Promoting Phorbol Esters to Protein Kinase C

Yusushi Tanaka; Ryohei Miyake; Ushio Kikkawa; Yasutomi Nishizuka


Japanese Circulation Journal-english Edition | 1989

-171-CHARACTERIZATION OF PHOSPHOLIPASE A_2 IN VASCULAR SMOOTH MUSCLE : Cardiac Metabolism, Cardiac Biochemistry : FREE COMMUNICATIONS(I) : PROCEEDINGS OF THE 53th ANNUAL SCIENTIFIC MEETING OF THE JAPANESE CIRCULATION SOCIETY

Ryohei Miyake; Hozuka Akita; Mitsuhiro Yokoyama; Hisashi Fukuzaki


Japanese Circulation Journal-english Edition | 1990

-0917-EFFECTS OF VASOACTIVE INTESTINAL PEPTIDE ON CORONARY CIRCULATION : COMPARISON WITH SUBSTANCE P : THE 54th ANNUAL SCIENTIFIC MEETING OF THE JAPANESE CIRCULATION SOCIETY

Yuichi Matsuda; Mitsuhiro Yokoyama; Nobutaka Inoue; Akito Yatani; Ken-ichi Hirata; Yasuo Hamamori; Ryohei Miyake; Hozuka Akita; Hisashi Fukuzaki


Japanese Circulation Journal-english Edition | 1990

-0620-LYSOPHOSPHATIDYLCHOLINE : ESSENTIAL ROLE IN THE INHIBITION OF ENDOTHELIUM-DEPENDENT VASORELAXATION BY OXIDIXED LOW DENSITY LIPOPROTEIN

Ken-ichi Hirata; Mitsuhiro Yokoyama; Hozuka Akita; Ryohei Miyake; Yuichi Matsuda; Nobutaka Inoue; Hisashi Fukuzaki


Japanese Circulation Journal-english Edition | 1990

-0621-ALTERATION OF VASCULAR TONE BY LYSOPHOSPHATIDYLCHOLINE (LYSOPC) IN RABBIT AORTA

Ryohei Miyake; Mitsuhiro Yokoyama; Ken-ichi Hirata; Mitsuhiko Yamada; Hozuka Akita; Hisashi Fukuzaki


Japanese Circulation Journal-english Edition | 1989

P_2-PURINERGIC RECEPTOR MEDIATED PHOSPHOINOSITIDES (PI) METABOLISM IN CULTURED FETAL CARDIAC MYOCYTES : Myocardial Metabolism, Biochemistry : 53 Annual Scientific Meeting, Japanese Circulation Society

Mitsuhiko Yamada; Mitsuhiro Yokoyama; Yasuo Hamamori; Ryohei Miyake; Yuichi Matsuda; Ken-ichi Hirata; Akiko Yatani; Hozuka Akita; Hisashi Fukuzaki

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