鸢尾酮通过表观遗传调控 Nrf2 介导的 ROS 清除来抑制破骨细胞生成,并对抗 OVX 诱导的骨质疏松症。
Damascenone inhibits osteoclastogenesis by epigenetically modulating Nrf2-mediated ROS scavenge and counteracts OVX-induced osteoporosis.
机构信息
Department of Orthopedics, Qilu Hospital of Shandong University, Jinan, Shandong, China.
Department of Orthopedics, Qilu Hospital of Shandong University, Jinan, Shandong, China; Cheeloo College of Medicine, Shandong University, Jinan, Shandong, China.
出版信息
Phytomedicine. 2024 Dec;135:156205. doi: 10.1016/j.phymed.2024.156205. Epub 2024 Nov 3.
BACKGROUND
Bone formation and resorption regulate bone homeostasis. Excessive osteoclastogenesis enhances bone resorption and causes osteoporosis. Although medicines targeting osteoclast have been developed, these drugs have several side effects. Natural compounds have advantages in safety and efficiency, making them potential candidates for osteoporosis treatment.
PURPOSE
This study aims to elucidate the role of damascenone (Dama) in osteoclastogenesis and osteoporosis.
STUDY DESIGN AND METHODS
To demonstrate the effect of Dama on osteoclast differentiation and function, we performed multiple in vitro experiments including TRAP staining, F-actin staining, bone slice resorption assay, real-time PCR, and western bolt. Further, ROS detection, network pharmacology, microscale thermophoresis assay, and ChIP assay were conducted to elucidate the underlying molecular mechanism. Finally, the in vivo effects of Dama were verified using an ovariectomy induced osteoporosis mice model.
RESULTS
Dama inhibited RANKL-induced osteoclast differentiation and bone resorptive function in vitro. The expression of osteoclast-related genes and activation of MAPKs and NF-κB signaling in osteoclast were also attenuated by Dama. Meanwhile, Dama reduced intracellular ROS level via up-regulating Nrf2 expression. Network pharmacology demonstrated that HDAC2 is the potential direct target of Dama. Dama inhibited HDAC2 function and increased H3K27ac level of Nrf2, which induced Nrf2 expression and activated ROS scavenging enzymes. Inhibiting NRF2 or activating HDAC2 attenuated the effect of Dama on osteoclastogenesis. Finally, Dama injection suppressed in vivo osteoclastogenesis and ameliorated bone loss induced by OVX.
CONCLUSION
Dama attenuates osteoclastogenesis by epigenetically modulating Nrf2 expression and ROS scavenge. This study provides evidence for Dama being a potential treatment for osteoporosis.
背景
骨形成和吸收调节着骨稳态。破骨细胞过度生成会增强骨吸收,导致骨质疏松症。虽然已经开发出针对破骨细胞的药物,但这些药物有许多副作用。天然化合物在安全性和效率方面具有优势,使其成为治疗骨质疏松症的潜在候选药物。
目的
本研究旨在阐明大马酮(Dama)在破骨细胞生成和骨质疏松症中的作用。
研究设计和方法
为了证明 Dama 对破骨细胞分化和功能的影响,我们进行了多项体外实验,包括 TRAP 染色、F-actin 染色、骨片吸收测定、实时 PCR 和 Western blot。此外,还进行了 ROS 检测、网络药理学、微量热泳动测定和 ChIP 测定,以阐明潜在的分子机制。最后,使用卵巢切除诱导的骨质疏松症小鼠模型验证了 Dama 的体内作用。
结果
Dama 抑制了体外 RANKL 诱导的破骨细胞分化和骨吸收功能。Dama 还减弱了破骨细胞中与破骨细胞相关的基因表达和 MAPKs 和 NF-κB 信号通路的激活。同时,Dama 通过上调 Nrf2 表达来降低细胞内 ROS 水平。网络药理学表明,HDAC2 是 Dama 的潜在直接靶标。Dama 抑制了 HDAC2 的功能,增加了 Nrf2 的 H3K27ac 水平,诱导了 Nrf2 的表达并激活了 ROS 清除酶。抑制 NRF2 或激活 HDAC2 减弱了 Dama 对破骨细胞生成的作用。最后,Dama 注射抑制了体内破骨细胞生成,并改善了 OVX 诱导的骨丢失。
结论
Dama 通过表观遗传调节 Nrf2 表达和 ROS 清除来抑制破骨细胞生成。本研究为 Dama 作为骨质疏松症潜在治疗方法提供了证据。
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