Document Type
Article
Publication Date
9-1-2024
Department
Department of Chemistry
Abstract
Over the last decades, the increased incidence of metabolic disorders, such as type two diabetes and obesity, has motivated researchers to investigate new enzyme inhibitors. Inhibition of the α-amylase enzyme is one therapeutic approach in lowering glucose levels in the blood to manage diabetes mellitus. The objective of this study was to synthesize short α-/β-mixed peptides in the solution phase. The Boc-protected α-L-leucine was converted to β-analogue by using Arndt–Eistert synthesis with the advantage of no racemization and retention of configuration. Three novel short peptides were successfully synthesized: N(Boc)-Gly-β-Leu–OCH3(14), N(Boc)-O(Bz)α-Ser-β-Leu–OCH3(16), and N(Boc)-O(Bz)-α-Tyr-α-Gly-β-Leu–OCH3(17), characterized by FTIR and 1H NMR analysis. The synthesized peptide 16 showed highest inhibitory activity (45.22%) followed by peptide 14 (18.51%) and peptide 17 (17.05%), respectively. Intriguingly, peptide 16 showed higher inhibition on α-amylase compared with other α-/β-mixed peptides.
Publication Title
Molecules
Recommended Citation
Ahmed, N.,
Razzaq, F.,
Arfan, M.,
Gatasheh, M.,
Nasir, H.,
Ali, J.,
&
Hafeez, H.
(2024).
A Convenient Synthesis of Short α-/β-Mixed Peptides as Potential α-Amylase Inhibitors.
Molecules,
29(17).
http://doi.org/10.3390/molecules29174028
Retrieved from: https://digitalcommons.mtu.edu/michigantech-p2/1091
Creative Commons License
This work is licensed under a Creative Commons Attribution 4.0 International License.
Version
Publisher's PDF
Publisher's Statement
Copyright: © 2024 by the authors. Licensee MDPI, Basel, Switzerland. Publisher’s version of record: https://doi.org/10.3390/molecules29174028