TY - JOUR
T1 - Rational Design and Synthesis of Novel Benzimidazole Derivatives as Potential β-Glucosidase Inhibitors
AU - Liu, Xu
AU - Sun, Ge
AU - Li, Fengxing
AU - Feng, Xia
AU - Jia, Tongguan
AU - Luo, Cheng
AU - Chen, Shijie
AU - Chen, Hua
N1 - Publisher Copyright:
© 2024 Bentham Science Publishers.
PY - 2024
Y1 - 2024
N2 - Background: β-Glucosidase has a variety of biological functions. A structural model for a potential β-glucosidase inhibitor has been proposed in the studies. Objective: A series f new diaryl derivatives linked through benzimidazole have been randomly and rationally designed, synthesized, and evaluated for their inhibitory activities against β-glucosidase (al-mond). The proposed structural model provides a new strategy for the design of potent β-glucosidase inhibitors. Methods: According to the model, a series of benzimidazole derivatives were designed and synthesized, and their inhibitory activity, Ki value, inhibitory type, and binding mode analysis (PDB ID: 2J7C) on β-glucosidase (almond) were evaluated. Results: Two compounds 7b and 7d were the best inhibitors with IC50 values of 7.86 µM and 3.52 µM, respectively. Their Ki values were calculated to be 9.91 µM and 5.81 µM, respectively. Conclusion: The SAR analysis suggested that such benzimidazole derivatives might bind to the active site of β-glucosidase mainly through hydrogen bonds on o-trihydroxyphenol; the additional phenyl ring on the other side towards the solvent-exposed region played a very important role in improving their in-hibitory activity against β-glucosidase.
AB - Background: β-Glucosidase has a variety of biological functions. A structural model for a potential β-glucosidase inhibitor has been proposed in the studies. Objective: A series f new diaryl derivatives linked through benzimidazole have been randomly and rationally designed, synthesized, and evaluated for their inhibitory activities against β-glucosidase (al-mond). The proposed structural model provides a new strategy for the design of potent β-glucosidase inhibitors. Methods: According to the model, a series of benzimidazole derivatives were designed and synthesized, and their inhibitory activity, Ki value, inhibitory type, and binding mode analysis (PDB ID: 2J7C) on β-glucosidase (almond) were evaluated. Results: Two compounds 7b and 7d were the best inhibitors with IC50 values of 7.86 µM and 3.52 µM, respectively. Their Ki values were calculated to be 9.91 µM and 5.81 µM, respectively. Conclusion: The SAR analysis suggested that such benzimidazole derivatives might bind to the active site of β-glucosidase mainly through hydrogen bonds on o-trihydroxyphenol; the additional phenyl ring on the other side towards the solvent-exposed region played a very important role in improving their in-hibitory activity against β-glucosidase.
KW - benzimidazole
KW - iminosugar
KW - linker
KW - o-trihydroxyphenol
KW - solvent-exposed region
KW - β-glucosidase inhibitors
UR - https://www.scopus.com/pages/publications/85201711702
U2 - 10.2174/1570180820666230822141514
DO - 10.2174/1570180820666230822141514
M3 - 文章
AN - SCOPUS:85201711702
SN - 1570-1808
VL - 21
SP - 2674
EP - 2683
JO - Letters in Drug Design and Discovery
JF - Letters in Drug Design and Discovery
IS - 13
ER -