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Chemical constituents of Himantormia lugubris collected from Antarctica and their PTP1B and α-glucosidase inhibitory activities

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Title
Chemical constituents of Himantormia lugubris collected from Antarctica and their PTP1B and α-glucosidase inhibitory activities
Other Titles
남극지의류, Himantormia lugubris로 부터 화학성분들 및 이들의 항당뇨 활성
Authors
Ha Manh Tuan
Le Thi Thanh
Lee Da Yeong
Kim Chung Sub
Youn, Ui Joung
Kim, Sanghee
Kim Jeong Ah
Min Byung Sun
Keywords
Himantormia lugubrisLanostane-type triterpenoidPTP1Bα-glucosidaseParmeliaceae
Issue Date
2025
Citation
Ha Manh Tuan, et al. 2025. "Chemical constituents of Himantormia lugubris collected from Antarctica and their PTP1B and α-glucosidase inhibitory activities". Phytochemistry Letters, 66(0): 91-99.
Abstract
A phytochemical investigation of an Antarctic endemic species [Himantormia lugubris (Hue) M. Lamb] led to the isolation and structural elucidation of three new compounds including one lanostane-type triterpenoid (1, himanlugubrol A), one ergostane-type sterol (2, himanlugubrol B), one benzyl orsellinate derivative (3, himanlugubrin A), along with ten known compounds (4-13). The chemical structures of new compounds were determined using diverse NMR techniques, HRESIMS data analysis, and computational approaches supported by advanced statistics (DP4+). The anti-diabetic potential of all isolated compounds was investigated by evaluating their inhibitory effects on PTP1B and alpha-glucosidase enzymes. As a result, compound 3 moderately inhibited PTP1B with an IC50 value of 43.86 mu M and significantly inhibited alpha-glucosidase (IC50 = 73.46 mu M) in comparison to the positive controls, ursolic acid (IC50 = 5.92 mu M) and acarbose (IC50 = 210.11 mu M), respectively. Enzyme kinetic analysis revealed that compound 3 demonstrated noncompetitive inhibition of PTP1B and mixed-type inhibition of alpha-glucosidase. Additionally, molecular docking results supported these in vitro findings, showing that compound 3 had strong binding affinities for the active sites of both PTP1B and alpha-glucosidase, indicated by the key H-bond and van der Waals interactions and negative binding energies.
URI
https://repository.kopri.re.kr/handle/201206/16439
DOI
http://dx.doi.org/10.1016/j.phytol.2025.02.009
Type
Article
Station
King Sejong Station
Indexed
SCIE
Appears in Collections  
2018-2018, Large-scale production and Clinical evaluation of CPS (Cell-Protecting Substance) from polar microalgae (18-18) / Kim, Sanghee (PE18180)
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