Cannabinoid Receptor Type II Ligands from Sandalwood Oil and Synthetic α-Santalol Derivatives

IF 3.3 2区生物学 Q2 CHEMISTRY, MEDICINAL

Journal of Natural Products Pub Date : 2023-07-14 DOI:10.1021/acs.jnatprod.3c00282

Pradeep Paudel, Pankaj Pandey, Jason J. Paris, Nicole M. Ashpole, Fakhri Mahdi, Jun-Mian Tian, Joseph Lee, Mei Wang, Min Xu, Amar G. Chittiboyina, Ikhlas A. Khan, Samir A. Ross and Xing-Cong Li*,

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引用次数: 0

Abstract

Bioassay-guided fractionation of the essential oil of Santalum album led to the identification of α-santalol (1) and β-santalol (2) as new chemotypes of cannabinoid receptor type II (CB₂) ligands with K_i values of 10.49 and 8.19 μM, respectively. Nine structurally new α-santalol derivatives (4a–4h and 5) were synthesized to identify more selective and potent CB₂ ligands. Compound 4e with a piperazine structural moiety demonstrated a K_i value of 0.99 μM against CB₂ receptor and did not show binding activity against cannabinoid receptor type I (CB₁) at 10 μM. Compounds 1, 2, and 4e increased intracellular calcium influx in SH-SY5Y human neuroblastoma cells that were attenuated by CB₂ antagonism or inverse agonism, supporting the results that these compounds are CB₂ agonists. Molecular docking showed that 1 and 4e had similar binding poses, exhibiting a unique interaction with Thr114 within the CB₂ receptor, and that the piperazine structural moiety is required for the binding affinity of 4e. A 200 ns molecular dynamics simulation of CB₂ complexed with 4e confirmed the stability of the complex. This structural insight lays a foundation to further design and synthesize more potent and selective α-santalol-based CB₂ ligands for drug discovery.

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檀香油中大麻素受体II型配体及合成α-桑他洛尔衍生物

采用生物测定法对桑檀香精油进行分离，鉴定出α-桑檀香(1)和β-桑檀香(2)为大麻素受体II型(CB2)配体的新化学型，Ki值分别为10.49和8.19 μM。合成了9个结构上新的α-桑他洛尔衍生物(4a-4h和5)，以鉴定更具选择性和有效的CB2配体。含有哌嗪结构片段的化合物4e对CB2受体的Ki值为0.99 μM，对CB1型大麻素受体(CB1)在10 μM处无结合活性。化合物1、2和4e增加了SH-SY5Y人神经母细胞瘤细胞内钙内流，这些细胞被CB2拮抗剂或逆激动剂减弱，支持了这些化合物是CB2激动剂的结果。分子对接表明，1和4e具有相似的结合姿态，与CB2受体内的Thr114具有独特的相互作用，并且4e的结合亲和力需要哌嗪结构片段。对CB2与4e配合物进行了200 ns的分子动力学模拟，证实了配合物的稳定性。这为进一步设计和合成更有效和选择性的α-桑他洛尔基CB2配体用于药物发现奠定了基础。

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来源期刊

Journal of Natural Products 生物-药学

CiteScore

9.10

自引率

5.90%

发文量

294

审稿时长

2.3 months

期刊介绍： The Journal of Natural Products invites and publishes papers that make substantial and scholarly contributions to the area of natural products research. Contributions may relate to the chemistry and/or biochemistry of naturally occurring compounds or the biology of living systems from which they are obtained. Specifically, there may be articles that describe secondary metabolites of microorganisms, including antibiotics and mycotoxins; physiologically active compounds from terrestrial and marine plants and animals; biochemical studies, including biosynthesis and microbiological transformations; fermentation and plant tissue culture; the isolation, structure elucidation, and chemical synthesis of novel compounds from nature; and the pharmacology of compounds of natural origin. When new compounds are reported, manuscripts describing their biological activity are much preferred. Specifically, there may be articles that describe secondary metabolites of microorganisms, including antibiotics and mycotoxins; physiologically active compounds from terrestrial and marine plants and animals; biochemical studies, including biosynthesis and microbiological transformations; fermentation and plant tissue culture; the isolation, structure elucidation, and chemical synthesis of novel compounds from nature; and the pharmacology of compounds of natural origin.