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Research Field (Keyword)
Publications
(Last updated : 2024-02-20 08:41:21)
SEKIYA Hiroshi
Department
Matsuyama University School of Clinical Pharmacy, College of Pharmaceutical Sciences
Position
Associate professor
Research Field (Keyword)
Bacteriology (includes mycology)
Publications
1.
2023/11
Article
Biochemical Characterizations of the Putative Amidase Endolysin Ecd18980 Catalytic Domain from
Clostridioides difficile
(Collaboration)
2.
2023/03
Article
Structural and biochemical characterization of
Clostridium perfringens pili
protein B collagen-binding domains (Collaboration)
3.
2022/08
Article
Biochemical Characterizations of the Putative Endolysin Ecd09610 Catalytic Domain from
Clostridioides difficile
(Collaboration)
4.
2021/10
Article
Structural and biochemical characterization of the
Clostridium perfringens
-specific Zn
2+
-dependent amidase endolysin, Psa, catalytic domain (Collaboration)
5.
2021/05
Article
X-ray structures of Clostridium perfringens sortase C with C-terminal cell wall sorting motif of LPST demonstrate role of subsite for substrate-binding and structural variations of catalytic site. (Collaboration)
6.
2021/04
Article
Structural and biochemical characterizations of the novel autolysin Acd24020 from Clostridioides difficile and its full-function catalytic domain as a lytic enzyme. (Collaboration)
7.
2021/03
Article
A Putative Amidase Endolysin Encoded by Clostridium perfringens St13 Exhibits Specific Lytic Activity and Synergizes with the Muramidase Endolysin Psm (Collaboration)
8.
2020/09
Article
Benzoxazole-Based Metal Complexes to Reverse Multidrug Resistance in Bacteria. (Collaboration)
9.
2019/08
Article
Structures of major pilins in Clostridium perfringens demonstrate dynamic conformational change. (Collaboration)
10.
2018/11
Article
Benzoxazole-based Zn(II) and Cu(II) Complexes Overcome Multidrug-resistance in Cancer. (Collaboration)
11.
2018
Article
Synthesis and antimicrobial activity of 2-trifluoroacetonylbenzoxazole ligands and their metal complexes (Collaboration)
12.
2017/11
Article
X-ray structure of Clostridium perfringens sortase B cysteine transpeptidase (Collaboration)
13.
2017/09
Article
Identification of Characteristic Phenolic Constituents in Mousouchiku Extract Used as Food Additives (Collaboration)
14.
2017/04
Article
A Novel Methodology for Synthesis of 1,5,6-Trisubstituted 2(1H)-Pyrazinones of Biological Interest (Collaboration)
15.
2017/01
Article
Structural and biochemical characterization of the Clostridium perfringens autolysin catalytic domain (Collaboration)
16.
2014/12
Other
The visual recognition of parasitic helminths in Japan before the introduction of parasitology from Germany-A preliminary note on the confirmation from Jomon Period onward (Collaboration)
17.
2014/04
Article
X-ray structure of a novel endolysin encoded by episomal phage phiSM101 of Clostridium perfringens (Collaboration)
18.
2011/01
Article
Identification and characterization of a putative endolysin encoded by episomal phage phiSM101 of Clostridium perfringens. (Collaboration)
19.
2010/03
Article
A growing need for international cooperative studies to establish medicinal-plant therapy against obstinate and biohazardous nematodes in the tropical and subtropical areas and in Japan (Collaboration)
20.
2009/08
Article
Gene cloning and characteristics of the RND-type multidrug efflux pump MuxABC-OpmB possessing two RND components in Pseudomonas aeruginosa. (Collaboration)
21.
2009/06
Article
Infections with gastrointestinal parasitic helminths indigenous to Japan and their treatment historically studied in an attempt to control the diseases in countries where they are still rampant: (1) the Jomon to Edo periods. (Collaboration)
22.
2008/12
Article
Construction of the curriculum and lectures for the subject, "History of pharmacy" in Matsuyama University School of Pharmacy. (Collaboration)
23.
2005/11
Article
Gene cloning and properties of the RND-type multidrug efflux pumps MexPQ-OpmE and MexMN-OprM from Pseudomonas aeruginosa. (Collaboration)
24.
2003/09
Article
Functional cloning and characterization of a multidrug efflux pump, MexHI-OpmD, from a Pseudomonas aeruginosa mutant. (Collaboration)
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