Issue 6, 2021
From the journal:

RSC Advances

Ligand compatibility of salacinol-type α-glucosidase inhibitors toward the GH31 family

Fumihiro Ishikawa, ORCID logo a   Aiko Hirano,a   Yuuto Yoshimori,a   Kana Nishida,a   Shinya Nakamura,b   Katsuki Takashima,a   Shinsuke Marumoto,c   Kiyofumi Ninomiya,d   Isao Nakanishi,b   Weijia Xie,e   Toshio Morikawa, ORCID logo d   Osamu Muraokad  and  Genzoh Tanabe ORCID logo *ad  

* Corresponding authors

a Pharmaceutical Organic Chemistry Lab, Faculty of Pharmacy, Kindai University, 3-4-1 Kowakae, Higashi-Osaka, Osaka 577-8502, Japan

b Computational Drug Design and Discovery Lab, Faculty of Pharmacy, Kindai University, 3-4-1 Kowakae, Higashi-Osaka, Osaka 577-8502, Japan

c Joint Research Center, Kindai University, 3-4-1 Kowakae, Higashi-Osaka, Osaka 577-8502, Japan

d Pharmaceutical Research and Technology Institute, Kindai University, 3-4-1 Kowakae, Higashi-Osaka, Osaka 577-8502, Japan

e State Key Laboratory of Natural Medicines, Department of Medicinal Chemistry, China Pharmaceutical University, Nanjing 2100009, P. R. China
E-mail: g-tanabe@phar.kindai.ac.jp

Abstract

We show that salacinol-type α-glucosidase inhibitors are ligand-compatible with the GH 31 family. Salacinol and its 3′-O-benzylated analogs inhibit human lysosomal α-glucosidase at submicromolar levels. Simple structure-activity relationship studies reveal that the salacinol side-chain stereochemistry significantly influences binding to GH31 α-glucosidases.

Graphical abstract: Ligand compatibility of salacinol-type α-glucosidase inhibitors toward the GH31 family

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Article information

DOI
https://doi.org/10.1039/D0RA10038B
Article type
Paper
Submitted
27 nov. 2020
Accepted
28 déc. 2020
First published
15 janv. 2021
This article is Open Access
Creative Commons BY-NC license

RSC Adv., 2021,11, 3221-3225

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Ligand compatibility of salacinol-type α-glucosidase inhibitors toward the GH31 family

F. Ishikawa, A. Hirano, Y. Yoshimori, K. Nishida, S. Nakamura, K. Takashima, S. Marumoto, K. Ninomiya, I. Nakanishi, W. Xie, T. Morikawa, O. Muraoka and G. Tanabe, RSC Adv., 2021, 11, 3221 DOI: 10.1039/D0RA10038B

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