Characterization of Recombinant Human Chymase Expressed in Escherichia coli
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概要
- 論文の詳細を見る
We compared recombinant human chymase expressed in Escherichia coli with human chymase purified from vascular tissues.The recombinant chymase, the structure of which was NH2-enterokinase cleavage site-chymase-COOH, was expressed in Escherichia coli and then was solubilized and renatured.The protein did not have a chymase activity, but gained this activity after the cleavage of the N-terminal site by enterokinase.The enzyme was purified by heparin affinity and gel filtration columns.The N-terminal sequence of the protein was identical to the sequence for human chymase.The molecular weights of the recombinant chymase and chymase purified from human vascular tissues were 26 and 30kDa, respectively, and the 4kDa difference was thought to be due to the presence or absence of glycan.The optimum pH of the recombinant enzyme activity was between 7.5 and 9.0.The activity of the recombinant enzyme was inhibited by chymostatin, soybean trypsin inhibitor and phenylmethylsulfonyl fluoride, but not by ethylenediaminetetraacetic acid and aprotinin.This enzyme cleaved specifically the Phe8-His9 bond of angiotensin(Ang)I to form Ang II and that of big endothelin(ET)-1 to form ET-1-(1-31).These findings demonstrated that the enzymatic characteristics of the recombinant enzyme were identical to that of native human chymase.
- 社団法人 日本薬理学会の論文
- 2000-02-01
著者
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Takai Shinji
Department Of Cardiology Kouseikai Takeda Hospital
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Sakaguchi Minoru
大阪薬科大学
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Sakaguchi Minoru
Intensive Grazing Research Team National Agricultural Research Center For Hokkaido Region National A
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Matsumura E
大阪医科大学 薬理
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JIN Denan
Department of Pharmacology, Osaka Medical College
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MIYAZAKI Mizuo
Department of Pharmacology, Osaka Medical College
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Matsumura Eiko
大阪医科大学 薬理
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Takai Shinji
Department Of Pharmacology Osaka Medical College
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SUMI Shin-ichiro
Institute for Biotechnology Research, Wakunaga Pharmaceutical Co., Itd
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AOIKE Masaki
Institute for Biotechnology Research, Wakunaga Pharmaceutical Co., Itd
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SAKAGUCHI Masato
Department of Pharmacology, Osaka Medical College
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ITOH Yoshimi
Department of Cell Biology, Osaka University of Pharmaceutical Co., Ltd
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MATSUMURA Eiko
Department of Cell Biology, Osaka University of Pharmaceutical Co., Ltd
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Sasaki Shinjiro
Department Of Thoracic And Cardiovascular Surgery
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Jin Denan
Department Of Pharmacology Osaka Medical College
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Matsumura Eiko
Department Of Cell Biology Osaka University Of Pharmaceutical Co. Ltd
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Sakaguchi M
Laboratory Of Cell Biology Osaka University Of Pharmaceutical Sciences
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Sasaki Shinjiro
Department Of Thoracic And Cardiovascular Surgery Osaka Medical College
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Miyazaki Mizuo
Department Of Pharmacology Osaka Medical College Takatsuki City
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Aoike Masaki
Institute For Biotechnology Research Wakunaga Pharmaceutical Co. Itd
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Itoh Y
Department Of Cell Biology Osaka University Of Pharmaceutical Co. Ltd
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Sumi Shin-ichiro
Thoracic And Cardiovascular Surgery Osaka Medical College
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Miyazaki Mizuo
Department Of Pharmacoldgy Osaka Medical College
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Tanda Syuji
Division Of Hypertension And Nephrology Department Of Internal Medicine Kyoto Prefectural University
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Sumi Shin-ichiro
Institute For Biotechnology Research Wakunaga Pharmaceutical Co. Itd
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Sakaguchi Masato
Department Of Materials Science & Technology Nagoya Institute Of Technology
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Takai Shinji
Department Of Animal Hygiene School Of Veterinary Medicine And Animal Sciences Kitasato University
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Sasaki Shinjiro
Department Of Thoraclc Surgery Osaka Medical College
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Sasaki Shinjiro
Dept. Of Surg. Osaka Med. Coll.
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MATSUMURA Eiko
Department of Agricultural Chemistry, College of Agriculture, University of Osaka Prefecture
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