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Flindissone, a Limonoid Isolated from Trichilia prieuriana, Is an LXR Agonist.


ABSTRACT: In this study, the ability of six limonoids from Trichilia prieuriana (Meliaceae) to activate the liver X receptor (LXR) was assessed. One of these limonoids, flindissone, was shown to activate LXR by reporter-gene assays. Flindissone is a ring-intact limonoid, structurally similar to sterol-like LXR ligands. In endogenous cellular settings, flindissone showed an activity profile that is characteristic of LXR agonists. It induced cholesterol efflux in THP-1 macrophages by increasing the cholesterol transporter ABCA1 and ABCG1 gene expression. In HepG2 cells, flindissone induced the expression of IDOL, an LXR-target gene that is associated with the downregulation of the LDL receptor. However, unlike synthetic and similarly to sterol-based LXR agonists, flindissone did not induce the expression of the SREBP1c gene, a major transcription factor regulating de novo lipogenesis. Additionally, flindissone also appeared to be able to inhibit post-translational activation of SREBP1c. The results presented here reveal a natural product as a new LXR agonist and point to an additional property of T. prieuriana and other plant extracts containing flindissone.

SUBMITTER: Resetar M 

PROVIDER: S-EPMC10463221 | biostudies-literature | 2023 Aug

REPOSITORIES: biostudies-literature

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Flindissone, a Limonoid Isolated from <i>Trichilia prieuriana</i>, Is an LXR Agonist.

Resetar Mirta M   Tietcheu Galani Borris R BR   Tsamo Armelle T AT   Chen Ya Y   Schachner Daniel D   Stolzlechner Stefanie S   Mawouma Pagna Julio I JI   Beniddir Mehdi A MA   Kirchmair Johannes J   Dirsch Verena M VM  

Journal of natural products 20230801 8


In this study, the ability of six limonoids from <i>Trichilia prieuriana</i> (Meliaceae) to activate the liver X receptor (LXR) was assessed. One of these limonoids, flindissone, was shown to activate LXR by reporter-gene assays. Flindissone is a ring-intact limonoid, structurally similar to sterol-like LXR ligands. In endogenous cellular settings, flindissone showed an activity profile that is characteristic of LXR agonists. It induced cholesterol efflux in THP-1 macrophages by increasing the c  ...[more]

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