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. 2024 Nov:134:155951.
doi: 10.1016/j.phymed.2024.155951. Epub 2024 Aug 10.

Liquiritin exerts psoriasis therapy and prevention by regulating the YY1/RBP3 axis

Guoshu Deng  1 Yulin Zhang  1 Jiankun Song  2 Xiaoxuan Ma  1 Yue Luo  2 Xiaoya Fei  2 Jingsi Jiang  2 Yi Ru  2 Zongguang Tai  2 Quangang Zhu  2 Xin Ma  2 Le Kuai  1 Bin Li  3 Ying Zhang  4 Ying Luo  5
Affiliations

Liquiritin exerts psoriasis therapy and prevention by regulating the YY1/RBP3 axis

Guoshu Deng et al. Phytomedicine. 2024 Nov.

Abstract

Background: Psoriasis (PSO) poses a global health threat. The current research challenge in PSO is relapse. Liquiritin (LIQ), a major active compound from Glycyrrhiza inflata Batalin, has multiple pharmacological properties, including anti-inflammatory and anti-proliferative. Nonetheless, the precise mechanisms underlying LIQ's therapeutic actions in PSO and prevention abilities remain elusive.

Purpose: The present study aimed to delve into the potential to treat and prevent PSO and the mechanism of LIQ.

Methods: The anti-inflammatory and anti-proliferative effects of LIQ were studied in vitro with the HaCaT cell line. Then, Transcriptional analysis and bioinformatic analysis were used to determine the internal associations of the target set. Subsequently, functional experiment, luciferase report assay, ChIP-PCR, and immunohistochemical validation of clinical samples were performed to investigate the mechanism of LIQ. Finally, the anti-psoriatic effects and prevention abilities of LIQ were verified in vivo with imiquimod (IMQ)-induced PSO-like mouse models.

Results: Here, we identified differentially expressed genes in LIQ-stimulated HaCaT cells and Retinol-Binding Protein 3 (RBP3) as the core target, whereas YY1 was a predicted upstream transcription factor of RBP3. The YY1/RBP3 axis was obviously altered after administering LIQ at optimal doses of 20 μM in vitro and 100 µg/ml in vivo. LIQ can significantly inhibit the progression of PSO in vivo. Notably, LIQ also prevented the relapse of psoriatic lesions induced by the second round of low-dose IMQ. Mechanistically, we observed that LIQ could increase the promotion of YY1 for RBP3 by enhancing the binding affinity between them.

Conclusion: These findings revealed that the YY1/RBP3 axis is a potential psoriatic target, and LIQ is a promising and innovative therapeutic candidate for the treatment and prevention of PSO.

Keywords: Liquiritin; Psoriasis; Relapse; Retinol-binding protein 3; Transcriptional regulation; Yin Yang 1.

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Conflict of interest statement

Declaration of competing interest The authors declare that there are no conflicts of interest.

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