Murrayafoline A inhibits inflammatory cytokines in RAW264.7 cells stimulated with LPS and poly (I:C) by targeting the aryl hydrocarbon receptor

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DOI:

https://doi.org/10.3329/bjp.v20i1.80391

Keywords:

Aryl hydrocarbon receptor, Inflammatory cytokine , Lipopolysaccharide, Murrayafoline A , Poly (I:C), RAW264.7 cell, Glycosmis stenocarpa

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References

Bogunovic D, Manches O, Godefroy E, Yewdall A, Gallois A, Salazar AM, Marie I, Levy DE, Bhardwaj N. TLR4 engagement during TLR3-induced proinflammatory signaling in dendritic cells promotes IL-10-mediated suppression of antitumor immunity. Cancer Res. 2011; 71: 5467-76.

Cuong NM, Wilhelm H, Porzel A, Arnold N, Wessjohann L. 1-O-substituted derivatives of murrayafoline A and their antifungal properties. Nat Prod Res. 2008; 22: 1428-32.

Ding X, Jin S, Tong Y, Jiang X, Chen Z, Mei S, Zhang L, Billiar TR, Li Q. TLR4 signaling induces TLR3 up-regulation in alveolar macrophages during acute lung injury. Sci Rep. 2017; 7: 34278.

Ehrlich AK, Pennington JM, Bisson WH, Kolluri SK, Kerkvliet NI. TCDD, FICZ, and other high affinity AhR ligands dose-dependently determine the fate of CD4+ T cell differentiation. Toxicol Sci. 2018; 161: 310-20.

Gorskaya YF, Tukhvatulin AI, Dzharullaeva AS, Nesterenko VG. Combined administration of TLR4 (LPS) and TLR3 (Poly I:C) ligands to CBA mice elevates the content of osteogenic MSC by 1.6 times and increases content of bone marrow MSC to intermediate level between values attained by their individual administration. Bull Exp Biol Med. 2020; 168: 767-72.

Gruszczyk J, Grandvuillemin L, Lai-Kee-Him J, Paloni M, Savva CG, Germain P, Grimaldi M, Boulahtouf A, Kưong HS, Ancelin A, Bechara C, Barducci A, Balaguer P, Bourguet W. Cryo-EM structure of the agonist-bound Hsp90-XAP2-AHR cytosolic complex. Nat Commun. 2022; 13: 7010.

Hirano M, Hwang JH, Park HJ, Bak SM, Iwata H, Kim EY. In silico analysis of the interaction of avian aryl hydrocarbon receptors and dioxins to decipher isoform-, ligand-, and species-specific activations. Environ Sci Technol. 2015; 49: 3795-804.

Jiang W, Sun R, Wei H, Tian Z. Toll-like receptor 3 ligand attenuates LPS-induced liver injury by down-regulation of toll-like receptor 4 expression on macrophages. Proc Natl Acad Sci USA. 2005; 102: 17077-82.

Kimura A, Naka T, Nakahama T, Chinen I, Masuda K, Nohara K, Fujii-Kuriyama Y, Kishimoto T. Aryl hydrocarbon receptor in combination with Stat1 regulates LPS-induced inflammatory responses. J Exp Med. 2009; 206: 2027-35.

Li C, Chen P, Vadasz B, Ma L, Zhou H, Lang S, Freedman J, Ni H. Costimulation with LPS or poly I:C markedly enhances the anti-platelet immune response and severity of fetal and neonatal alloimmune thrombocytopenia. Thromb Hemost. 2013; 110: 1250-58.

Li M, Wang M, Wen Y, Zhang H, Zhao GN, Gao Q. Signaling pathways in macrophages: Molecular mechanisms and therapeutic targets. Med Comm. 2023; 4: e349.

Thuy TT, Cuong NM, Toan TQ, Thang NN, Tai BH, Nhiem NX, Hong HJ, Kim S, Legoupy S, Koh YS, Kim YH. Synthesis of novel derivatives of murrayafoline A and their inhibitory effect on LPS-stimulated production of pro-inflammatory cytokines in bone marrow-derived dendritic cells. Arch Pharm Res. 2013; 36: 832-39.

Tran DM, Tran TT, Nguyen NTT, Chu HH, Nakahama T, Nguyen NT. Anti-inflammatory activity of 9-hydroxycan-thin-6-one extracted from hairy-root cultures of Eurycoma longifolia potentially via aryl hydrocarbon receptor induction. Bangladesh J Pharmacol. 2022; 17: 102-04.

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Published

2025-04-25

How to Cite

Tran, Trang Thu, et al. “Murrayafoline A Inhibits Inflammatory Cytokines in RAW264.7 Cells Stimulated With LPS and Poly (I:C) by Targeting the Aryl Hydrocarbon Receptor”. Bangladesh Journal of Pharmacology, vol. 20, no. 1, Apr. 2025, pp. 35-39, doi:10.3329/bjp.v20i1.80391.

Issue

Vol. 20 No. 1 (2025)

Section

Letter to the Editor

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Copyright (c) 2025 Trang Thu Tran, Nguyen Manh Cuong, Nguyen Xuan Ha, Taisuke Nakahama, Nam Trung Nguyen

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