AZD8330诱导的cIAP1上调通过抑制RIP1相关坏死信号通路减轻骨关节炎进展。
Upregulation of cIAP1 induced by AZD8330 alleviates osteoarthritis progression by inhibiting the RIP1-associated necrosis signaling pathway.
作者信息
Qiu Jianxin, Zheng Xiaohang, Cai Guoping, Ye Jiajing, Jiang Ting, Chen Lihua, Li Ze, Gong Yuhang, Hong Zhenghua, Chen Haixiao
机构信息
Orthopedic Department, Taizhou Hospital Affiliated to Wenzhou Medical University, Linhai, China; Enze Medical Research Center, Taizhou Hospital Affiliated to Wenzhou Medical University, Linhai, China.
Orthopedic Department, Taizhou Hospital Affiliated to Wenzhou Medical University, Linhai, China; Enze Medical Research Center, Taizhou Hospital Affiliated to Wenzhou Medical University, Linhai, China.
出版信息
Int Immunopharmacol. 2023 Dec;125(Pt B):111169. doi: 10.1016/j.intimp.2023.111169. Epub 2023 Nov 8.
BACKGROUND
Osteoarthritis (OA) is a prevalent degenerative joint disease [1]. It has come to light that AZD8330 can suppress the generation of proinflammatory factors and deter the inflammatory response [2]. Given that inflammation is a primary causative factor in OA, it is posited that AZD8330 might exhibit superior efficacy in OA management.
METHODS
In this study, we investigated the potential of intraperitoneal injection of AZD8330 to retard the progression of osteoarthritis in a murine model with surgically induced medial meniscus destruction (DMM). Concurrently, we employed ATDC5 cartilage cells to dissect the mechanism through which AZD8330 inhibits the TNF-α-induced NF-κB signaling pathway via modulation of RIP1. The findings revealed that AZD8330 mitigated cartilage degradation and the inflammatory response, leading to a substantial reduction in OARSI scores among DMM mice treated with AZD8330. Mechanistically, AZD8330 functioned as a suppressor of the TNF-α-induced NF-κB/p65 signaling pathway by facilitating the phosphorylation activation of cIAP1-mediated RIP1. The combination of data from both in vivo and in vitro experiments supports the conclusion that AZD8330 can attenuate chondrocyte degradation, thereby alleviating OA, by regulating the NF-κB/P65 signaling pathway through modulation of RIP1 activity. Consequently, the utilization of AZD8330 may hold potential in the prophylaxis of osteoarthritis.
RESULTS
Our investigation delineates the role of AZD8330 in the regulation of inflammation in the context of OA treatment. Furthermore, we have unveiled that the inhibitory impact of AZD8330 on OA may hinge upon the activation of cIAP1, which in turn downregulates RIP1, thereby restraining the NF-κB/P65 signaling pathway. This study lends credence to the notion that AZD8330 may be a promising contender for osteoarthritis therapy.
CONCLUSIONS
Our study provides compelling evidence attesting to the capacity of AZD8330 in managing inflammation within the realm of OA treatment. Likewise, our study has elucidated that the attenuation of OA by AZD8330 relies on the activation of cIAP1 to inhibit RIP1, consequently suppressing the NF-κB signaling pathway. On the strength of our present study, we may have identified a viable drug candidate for OA treatment.
背景
骨关节炎(OA)是一种常见的退行性关节疾病[1]。已发现AZD8330可抑制促炎因子的产生并阻止炎症反应[2]。鉴于炎症是OA的主要致病因素,推测AZD8330在OA治疗中可能具有卓越疗效。
方法
在本研究中,我们研究了腹腔注射AZD8330在手术诱导内侧半月板损伤(DMM)的小鼠模型中延缓骨关节炎进展的潜力。同时,我们使用ATDC5软骨细胞来剖析AZD8330通过调节RIP1抑制TNF-α诱导的NF-κB信号通路的机制。研究结果显示,AZD8330减轻了软骨降解和炎症反应,导致接受AZD8330治疗的DMM小鼠的OARSI评分大幅降低。机制上,AZD8330通过促进cIAP1介导的RIP1的磷酸化激活,作为TNF-α诱导的NF-κB/p65信号通路的抑制剂。体内和体外实验的数据结合支持了以下结论:AZD8330可通过调节RIP1活性来调控NF-κB/P65信号通路,从而减轻软骨细胞降解,进而缓解OA。因此,使用AZD8330可能在骨关节炎的预防中具有潜力。
结果
我们的研究阐述了AZD8330在OA治疗背景下对炎症调节的作用。此外,我们还发现AZD8330对OA的抑制作用可能取决于cIAP1的激活,cIAP1进而下调RIP1,从而抑制NF-κB/P65信号通路。本研究支持了AZD8330可能是骨关节炎治疗的一个有前景的候选药物这一观点。
结论
我们的研究提供了有力证据,证明AZD8330在OA治疗领域管理炎症的能力。同样,我们的研究阐明了AZD8330对OA的缓解依赖于激活cIAP1以抑制RIP1,从而抑制NF-κB信号通路。基于我们目前的研究,我们可能已经确定了一种用于OA治疗的可行候选药物。
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