| Literature DB >> 27325449 |
Genzoh Tanabe1, Weijia Xie2, Gorre Balakishan3, Mumen F A Amer4, Nozomi Tsutsui1, Haruka Takemura1, Shinya Nakamura1, Junji Akaki5, Kiyofumi Ninomiya5, Toshio Morikawa5, Isao Nakanishi1, Osamu Muraoka6.
Abstract
Using an in silico method, seven analogs bearing hydrophobic substituents (8a: Me, 8b: Et, 8c: n-Pent, 8d: n-Hept, 8e: n-Tridec, 8f: isoBu and 8g: neoPent) at the 3'-O-position in salacinol (1), a highly potent natural α-glucosidase inhibitor from Ayurvedic traditional medicine 'Salacia', were designed and synthesized. In order to verify the computational SAR assessments, their α-glucosidase inhibitory activities were evaluated in vitro. All analogs (8a-8g) exhibited an equal or considerably higher level of inhibitory activity against rat small intestinal α-glucosidases compared with the original sulfonate (1), and were as potent as or higher in potency than the clinically used anti-diabetics, voglibose, acarbose or miglitol. Their activities against human maltase exhibited good relationships to the results obtained with enzymes of rat origin. Among the designed compounds, the one with a 3'-O-neopentyl moiety (8g) was most potent, with an approximately ten fold increase in activity against human maltase compared to 1.Entities:
Keywords: In silico docking study; SAR study; Salacia; Salacinol; α-Glucosidase inhibitor
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Year: 2016 PMID: 27325449 DOI: 10.1016/j.bmc.2016.06.013
Source DB: PubMed Journal: Bioorg Med Chem ISSN: 0968-0896 Impact factor: 3.641