Novel harmine derivatives as potent acetylcholinesterase and amyloid beta aggregation dual inhibitors for management of Alzheimer’s disease

Hongtao DU; Jinzhi SONG; Fang MA; Hongxin GAO; Xinyan ZHAO; Renjun MAO; Xiaolong HE; Yan YAN

doi:10.1080/14756366.2023.2281893

Novel harmine derivatives as potent acetylcholinesterase and amyloid beta aggregation dual inhibitors for management of Alzheimer’s disease

Hongtao DU^*
, Jinzhi SONG
, Fang MA
, Hongxin GAO
, Xinyan ZHAO
, Renjun MAO
, Xiaolong HE
, Yan YAN^*

^*Corresponding author for this work

Research output: Journal Publications › Journal Article (refereed) › peer-review

10 Citations (Scopus)

Abstract

In this study, a series of potential ligands for the treatment of AD were synthesised and characterised as novel harmine derivatives modified at position 9 with benzyl piperazinyl. In vitro studies revealed that the majority of the derivatives exhibited moderate to potent inhibition against hAChE and Aβ₁₋₄₂ aggregation. Notably, compounds 13 and 17d displayed potent drug − likeness and ADMET properties, demonstrating remarkable inhibitory activities towards AChE (IC₅₀ = 58.76 nM and 89.38 nM, respectively) as well as Aβ aggregation (IC₅₀ = 9.31 μM and 13.82 μM, respectively). More importantly, compounds 13 and 17d showed exceptional neuroprotective effects against Aβ₁₋₄₂−induced SH − SY5Y damage, while maintaining low toxicity in SH − SY5Y cells. Further exploration of the mechanism through kinetic studies and molecular modelling confirmed that compound 13 could interact with both the CAS and the PAS of AChE. These findings suggested that harmine derivatives hold great potential as dual − targeted candidates for treating AD.

Original language	English
Article number	2281893
Number of pages	13
Journal	Journal of Enzyme Inhibition and Medicinal Chemistry
Volume	38
Issue number	1
Early online date	15 Nov 2023
DOIs	https://doi.org/10.1080/14756366.2023.2281893
Publication status	Published - 2023
Externally published	Yes

Bibliographical note

Publisher Copyright:
© 2023 The Author(s). Published by Informa UK Limited, trading as Taylor & Francis Group.

Funding

This work was supported by the Program for Natural Science Foundation of China] under Grant [No. 21602178]; [Qin Chuan Yuan cited the high-level innovation and entrepreneurship talent program of Shaanxi] under Grant [No. QCYRCXM-2022–172, QCYRCXM-2022–196]; and [Doctoral Research Initiation Project of Yan’an University] under Grant [No. 205040406, 205040422].

Keywords

acetylcholinesterase
Alzheimer’s disease
harmine
β−amyloid peptide

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title = "Novel harmine derivatives as potent acetylcholinesterase and amyloid beta aggregation dual inhibitors for management of Alzheimer{\textquoteright}s disease",

abstract = "In this study, a series of potential ligands for the treatment of AD were synthesised and characterised as novel harmine derivatives modified at position 9 with benzyl piperazinyl. In vitro studies revealed that the majority of the derivatives exhibited moderate to potent inhibition against hAChE and Aβ1 − 42 aggregation. Notably, compounds 13 and 17d displayed potent drug − likeness and ADMET properties, demonstrating remarkable inhibitory activities towards AChE (IC50 = 58.76 nM and 89.38 nM, respectively) as well as Aβ aggregation (IC50 = 9.31 μM and 13.82 μM, respectively). More importantly, compounds 13 and 17d showed exceptional neuroprotective effects against Aβ1 − 42−induced SH − SY5Y damage, while maintaining low toxicity in SH − SY5Y cells. Further exploration of the mechanism through kinetic studies and molecular modelling confirmed that compound 13 could interact with both the CAS and the PAS of AChE. These findings suggested that harmine derivatives hold great potential as dual − targeted candidates for treating AD.",

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author = "Hongtao DU and Jinzhi SONG and Fang MA and Hongxin GAO and Xinyan ZHAO and Renjun MAO and Xiaolong HE and Yan YAN",

note = "Publisher Copyright: {\textcopyright} 2023 The Author(s). Published by Informa UK Limited, trading as Taylor \& Francis Group.",

year = "2023",

doi = "10.1080/14756366.2023.2281893",

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T1 - Novel harmine derivatives as potent acetylcholinesterase and amyloid beta aggregation dual inhibitors for management of Alzheimer’s disease

AU - DU, Hongtao

AU - SONG, Jinzhi

AU - MA, Fang

AU - GAO, Hongxin

AU - ZHAO, Xinyan

AU - MAO, Renjun

AU - HE, Xiaolong

AU - YAN, Yan

PY - 2023

Y1 - 2023

N2 - In this study, a series of potential ligands for the treatment of AD were synthesised and characterised as novel harmine derivatives modified at position 9 with benzyl piperazinyl. In vitro studies revealed that the majority of the derivatives exhibited moderate to potent inhibition against hAChE and Aβ1 − 42 aggregation. Notably, compounds 13 and 17d displayed potent drug − likeness and ADMET properties, demonstrating remarkable inhibitory activities towards AChE (IC50 = 58.76 nM and 89.38 nM, respectively) as well as Aβ aggregation (IC50 = 9.31 μM and 13.82 μM, respectively). More importantly, compounds 13 and 17d showed exceptional neuroprotective effects against Aβ1 − 42−induced SH − SY5Y damage, while maintaining low toxicity in SH − SY5Y cells. Further exploration of the mechanism through kinetic studies and molecular modelling confirmed that compound 13 could interact with both the CAS and the PAS of AChE. These findings suggested that harmine derivatives hold great potential as dual − targeted candidates for treating AD.

AB - In this study, a series of potential ligands for the treatment of AD were synthesised and characterised as novel harmine derivatives modified at position 9 with benzyl piperazinyl. In vitro studies revealed that the majority of the derivatives exhibited moderate to potent inhibition against hAChE and Aβ1 − 42 aggregation. Notably, compounds 13 and 17d displayed potent drug − likeness and ADMET properties, demonstrating remarkable inhibitory activities towards AChE (IC50 = 58.76 nM and 89.38 nM, respectively) as well as Aβ aggregation (IC50 = 9.31 μM and 13.82 μM, respectively). More importantly, compounds 13 and 17d showed exceptional neuroprotective effects against Aβ1 − 42−induced SH − SY5Y damage, while maintaining low toxicity in SH − SY5Y cells. Further exploration of the mechanism through kinetic studies and molecular modelling confirmed that compound 13 could interact with both the CAS and the PAS of AChE. These findings suggested that harmine derivatives hold great potential as dual − targeted candidates for treating AD.

KW - acetylcholinesterase

KW - Alzheimer’s disease

KW - harmine

KW - β−amyloid peptide

UR - https://www.scopus.com/pages/publications/85177058645

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DO - 10.1080/14756366.2023.2281893

M3 - Journal Article (refereed)

AN - SCOPUS:85177058645

SN - 1475-6366

VL - 38

JO - Journal of Enzyme Inhibition and Medicinal Chemistry

JF - Journal of Enzyme Inhibition and Medicinal Chemistry

IS - 1

M1 - 2281893

ER -

Novel harmine derivatives as potent acetylcholinesterase and amyloid beta aggregation dual inhibitors for management of Alzheimer’s disease

Abstract

Bibliographical note

Funding

Keywords

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