Novel Non-carboxylate Benzoylsulfonamide-Based Protein Tyrosine Phosphatase 1B Inhibitors with Non-competitive Actions

Ko Morishita; Yoshimichi Shoji; Shunkichi Tanaka; Masaki Fukui; Yuma Ito; Tatsuya Kitao; Shin-ichiro Ozawa; Shuichi Hirono; Hiroaki Shirahase

doi:10.1248/cpb.c17-00635

Regular Articles

Novel Non-carboxylate Benzoylsulfonamide-Based Protein Tyrosine Phosphatase 1B Inhibitors with Non-competitive Actions

Ko Morishita, Yoshimichi Shoji, Shunkichi Tanaka, Masaki Fukui, Yuma Ito, Tatsuya Kitao, Shin-ichiro Ozawa, Shuichi Hirono, Hiroaki Shirahase

Author information

Ko Morishita
Drug Discovery Research Department, Kyoto Pharmaceutical Industries, Ltd.
Yoshimichi Shoji
Drug Discovery Research Department, Kyoto Pharmaceutical Industries, Ltd.
Shunkichi Tanaka
Drug Discovery Research Department, Kyoto Pharmaceutical Industries, Ltd.
Masaki Fukui
Drug Discovery Research Department, Kyoto Pharmaceutical Industries, Ltd.
Yuma Ito
Drug Discovery Research Department, Kyoto Pharmaceutical Industries, Ltd.
Tatsuya Kitao
Drug Discovery Research Department, Kyoto Pharmaceutical Industries, Ltd.
Shin-ichiro Ozawa
School of Pharmacy, Kitasato University
Shuichi Hirono
School of Pharmacy, Kitasato University
Hiroaki Shirahase Corresponding author
Drug Discovery Research Department, Kyoto Pharmaceutical Industries, Ltd.

Keywords: benzoylsulfonamide, protein tyrosine phosphatase 1B, allosteric inhibitor, non-competitive inhibitor, db/db mouse, Sprague-Dawley rat

JOURNAL FREE ACCESS FULL-TEXT HTML

2017 Volume 65 Issue 12 Pages 1144-1160

DOI https://doi.org/10.1248/cpb.c17-00635

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Abstract

A novel series of benzoylsulfonamide derivatives were synthesized and biologically evaluated. Among them, 4-(biphenyl-4-ylmethylsulfanylmethyl)-N-(hexane-1-sulfonyl)benzamide (compound 18K) was identified as a protein tyrosine phosphatase 1B (PTP1B) inhibitor with potent and selective inhibitory activity against PTP1B (IC₅₀=0.25 µM). Compound 18K functioned as a non-competitive inhibitor and bound to the allosteric site of PTP1B. It also showed high oral absorption in mice (the maximum drug concentration (C_max)=45.5 µM at 30 mg/kg), rats (C_max=53.6 µM at 30 mg/kg), and beagles (C_max=37.8 µM at 10 mg/kg), and significantly reduced plasma glucose levels at 30 mg/kg/d (per os (p.o.)) for one week with no side effects in db/db mice. In conclusion, the substituted benzoylsulfonamide was shown to be a novel scaffold of a non-competitive and allosteric PTP1B inhibitor, and compound 18K has potential as an efficacious and safe anti-diabetic drug as well as a useful tool for investigations of the physiological and pathophysiological effects of allosteric PTP1B inhibition.

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