CVClient

Koji Ichinose

  (市瀬 浩志)

Profile Information

Affiliation
Faculty of Pharmacy Department of Pharmaceutical Sciences, Musashino University
Degree
BSc(The University of Tokyo)
MSc(The University of Tokyo)
PhD(The University of Tokyo)

J-GLOBAL ID
200901070611481787
researchmap Member ID
1000202057

Papers

 82
  • Kazuki Ishikawa, Nao Kamiya, Masaki Ishii, Takashi Yaguchi, Koji Ichinose, Shinya Ohata
    Advances in Microbiology, 14(09) 448-467, Sep 29, 2024  Peer-reviewed
  • Masaki Ishii, Tsuyoshi Yamada, Kazuki Ishikawa, Koji Ichinose, Michel Monod, Shinya Ohata
    Antimicrobial agents and chemotherapy, e0160923, Apr 3, 2024  Peer-reviewed
    The increasing prevalence of dermatophyte resistance to terbinafine, a key drug in the treatment of dermatophytosis, represents a significant obstacle to treatment. Trichophyton rubrum is the most commonly isolated fungus in dermatophytosis. In T. rubrum, we identified TERG_07844, a gene encoding a previously uncharacterized putative protein kinase, as an ortholog of budding yeast Saccharomyces cerevisiae polyamine transport kinase 2 (Ptk2), and found that T. rubrum Ptk2 (TrPtk2) is involved in terbinafine tolerance. In both T. rubrum and S. cerevisiae, Ptk2 knockout strains were more sensitive to terbinafine compared with the wild types, suggesting that promotion of terbinafine tolerance is a conserved function of fungal Ptk2. Pma1 is activated through phosphorylation by Ptk2 in S. cerevisiae. Overexpression of T. rubrum Pma1 (TrPma1) in T. rubrum Ptk2 knockout strain (ΔTrPtk2) suppressed terbinafine sensitivity, suggesting that the induction of terbinafine tolerance by TrPtk2 is mediated by TrPma1. Furthermore, omeprazole, an inhibitor of plasma membrane proton pump Pma1, increased the terbinafine sensitivity of clinically isolated terbinafine-resistant strains. These findings suggest that, in dermatophytes, the TrPtk2-TrPma1 pathway plays a key role in promoting intrinsic terbinafine tolerance and may serve as a potential target for combinational antifungal therapy against terbinafine-resistant dermatophytes.
  • Koji Ichinose
    The Japanese Journal of Pharmacognosy, 78(1) 31-38, Feb, 2024  Peer-reviewedInvitedLead authorLast authorCorresponding author
  • Makoto Hashimoto, Susumu Watari, Takaaki Taguchi, Kazuki Ishikawa, Takuya Kumamoto, Susumu Okamoto, Koji Ichinose
    Angewandte Chemie (International ed. in English), 62(5) e202214400, Jan 26, 2023  Peer-reviewedLast authorCorresponding author
    A plethora of dimeric natural products exist with diverse chemical structures and biological activities. A major strategy for dimerization is aryl coupling reactions catalyzed by cytochrome P450 or laccase. Actinorhodin (ACT) from Streptomyces coelicolor has a dimeric pyranonaphthoquinone structure connected by a C-C bond. Here, we identified a NmrA-family dimerizing enzyme, ActVA-ORF4, and a cofactor independent oxidase, ActVA-ORF3, both involved in the last step of ACT biosynthesis. ActVA-ORF4 is a unique  NAD(P)H-dependent enzyme that catalyzes the inter-molecular C-C bond formation using 8-hydroxydihydrokalafungin (DHK-OH) as the sole substrate. On the other hand, ActVA-ORF3 was found to be a quinone-forming enzyme that produces the coupling substrate, DHK-OH, and the final product, ACT. Consequently, the functional assignment of all essential enzymes in ACT biosynthesis was completed, which would be a landmark in our understanding of the entire biosynthetic pathway for one of the best-known model natural products, ACT.
  • Kazuki Ishikawa, Makoto Hashimoto, Kunpei Komatsu, Takaaki Taguchi, Susumu Okamoto, Koji Ichinose
    Bioorganic & Medicinal Chemistry Letters, 66 128727-128727, Apr 9, 2022  Peer-reviewedLast authorCorresponding author
    Actinorhodin (ACT) is a benzoisochromanequinone antibiotic produced by Streptomyces coelicolor A3(2), which has served as a favored model organism for comprehensive studies of antibiotic biosynthesis and its regulation. (S)-DNPA undergoes various modifications as an intermediate in the ACT biosynthetic pathway, including enoyl reduction to DDHK. It has been suggested that actVI-ORF2 encodes an enoyl reductase (ER). However, its function has not been characterized in vitro. In this study, biochemical analysis of recombinant ActVI-ORF2 revealed that (S)-DNPA is converted to DDHK in a stereospecific manner with NADPH acting as a cofactor. (R)-DNPA was also reduced to 3-epi-DDHK with the comparable efficacy as (S)-DNPA, suggesting that the stereospecificity of ActVI-ORF2 was not affected by the stereochemistry at the C-3 of DNPA. ActVI-ORF2 is a new example of a discrete ER, which is distantly related to known ERs according to phylogenetic analysis.

Misc.

 129

Books and Other Publications

 6
  • 木内, 文之, 小松, かつ子, 三巻, 祥浩 (Role: Joint author, セリ科)
    南江堂, Feb, 2022 (ISBN: 9784524403882)
  • 竹谷, 孝一, 木内, 文之, 小松, かつ子 (Role: Joint author, セリ科)
    南江堂, Feb, 2018 (ISBN: 9784524403615)
  • 秋久, 俊博, 小池, 一男, 市瀬, 浩志, 浮谷, 基彦, 木村, 賢一, 佐藤, 忠章, 李, 巍, 木島, 孝夫, 羽野, 芳生, 堀田, 清, 増田, 和夫, 宮澤, 三雄, 安川, 憲 (Role: Joint author, 1序論;5生合成)
    共立出版, Apr, 2017 (ISBN: 9784320044524)
  • 竹田, 忠紘, 池城, 安正, 高橋, 邦夫, 斉藤, 和季, 小林, 義典(薬学) (Role: Joint author, ジテルペノイド;サポニン;天然由来の医薬品)
    廣川書店, Feb, 2017 (ISBN: 9784567431262)
  • 本多義昭;正山征洋;荻原幸夫;竹田忠紘 (Role: Joint author)
    南江堂, Apr, 2008 (ISBN: 9784524402410)

Presentations

 7

Professional Memberships

 4

Research Projects

 16