雷帕霉素通过抑制mTORC1并通过激活Akt诱导自噬来减轻炎症介导的椎间盘基质稳态失衡。
Rapamycin mitigates inflammation-mediated disc matrix homeostatic imbalance by inhibiting mTORC1 and inducing autophagy through Akt activation.
作者信息
Yurube Takashi, Buchser William J, Zhang Zhongying, Silwal Prashanta, Lotze Michael T, Kang James D, Sowa Gwendolyn A, Vo Nam V
机构信息
Ferguson Laboratory for Orthopaedic and Spine Research, Department of Orthopaedic Surgery University of Pittsburgh Medical Cancer, University of Pittsburgh Pittsburgh Pennsylvania USA.
Department of Orthopaedic Surgery Kobe University Graduate School of Medicine Kobe Japan.
出版信息
JOR Spine. 2024 Jan 2;7(1):e1303. doi: 10.1002/jsp2.1303. eCollection 2024 Mar.
BACKGROUND
Low back pain is a global health problem that originated mainly from intervertebral disc degeneration (IDD). Autophagy, negatively regulated by the phosphatidylinositol 3-kinase (PI3K)/Akt/mammalian target of rapamycin (mTOR) signaling pathway, prevents metabolic and degenerative diseases by removing and recycling damaged cellular components. Despite growing evidence that autophagy occurs in the intervertebral disc, the regulation of disc cellular autophagy is still poorly understood.
METHODS
Annulus fibrosus (rAF) cell cultures derived from healthy female rabbit discs were used to test the effect of autophagy inhibition or activation on disc cell fate and matrix homeostasis. Specifically, different chemical inhibitors including rapamycin, 3-methyladenine, MK-2206, and PP242 were used to modulate activities of different proteins in the PI3K/Akt/mTOR signaling pathway to assess IL-1β-induced cellular senescence, apoptosis, and matrix homeostasis in rAF cells grown under nutrient-poor culture condition.
RESULTS
Rapamycin, an inhibitor of mTOR complex 1 (mTORC1), reduced the phosphorylation of mTOR and its effector p70/S6K in rAF cell cultures. Rapamycin also induced autophagic flux as measured by increased expression of key autophagy markers, including LC3 puncta number, LC3-II expression, and cytoplasmic HMGB1 intensity and decreased p62/SQSTM1 expression. As expected, IL-1β stimulation promoted rAF cellular senescence, apoptosis, and matrix homeostatic imbalance with enhanced aggrecanolysis and MMP-3 and MMP-13 expression. Rapamycin treatment effectively mitigated IL-1β-mediated inflammatory stress changes, but these alleviating effects of rapamycin were abrogated by chemical inhibition of Akt and mTOR complex 2 (mTORC2).
CONCLUSIONS
These findings suggest that rapamycin blunts adverse effects of inflammation on disc cells by inhibiting mTORC1 to induce autophagy through the PI3K/Akt/mTOR pathway that is dependent on Akt and mTORC2 activities. Hence, our findings identify autophagy, rapamycin, and PI3K/Akt/mTOR signaling as potential therapeutic targets for IDD treatment.
背景
下腰痛是一个全球性的健康问题,主要源于椎间盘退变(IDD)。自噬受磷脂酰肌醇3激酶(PI3K)/蛋白激酶B(Akt)/雷帕霉素哺乳动物靶蛋白(mTOR)信号通路的负调控,通过清除和循环利用受损的细胞成分来预防代谢性和退行性疾病。尽管越来越多的证据表明自噬发生在椎间盘中,但对椎间盘细胞自噬的调控仍知之甚少。
方法
使用从健康雌性兔椎间盘获得的纤维环(rAF)细胞培养物来测试自噬抑制或激活对椎间盘细胞命运和基质稳态的影响。具体而言,使用包括雷帕霉素、3-甲基腺嘌呤、MK-2206和PP242在内的不同化学抑制剂来调节PI3K/Akt/mTOR信号通路中不同蛋白质的活性,以评估在营养匮乏培养条件下生长的rAF细胞中白细胞介素-1β(IL-1β)诱导的细胞衰老、凋亡和基质稳态。
结果
雷帕霉素是mTOR复合物1(mTORC1)的抑制剂,可降低rAF细胞培养物中mTOR及其效应器p70/S6K的磷酸化水平。雷帕霉素还通过增加关键自噬标志物的表达来诱导自噬流,这些标志物包括LC3斑点数量、LC3-II表达、细胞质高迁移率族蛋白B1(HMGB1)强度以及降低p62/ sequestosome 1(SQSTM1)表达。正如预期的那样,IL-1β刺激促进了rAF细胞衰老、凋亡和基质稳态失衡,伴有蛋白聚糖分解增加以及基质金属蛋白酶-3(MMP-3)和基质金属蛋白酶-13(MMP-13)表达增加。雷帕霉素处理有效地减轻了IL-1β介导的炎症应激变化,但雷帕霉素的这些缓解作用被Akt和mTOR复合物2(mTORC2)的化学抑制所消除。
结论
这些发现表明,雷帕霉素通过抑制mTORC1,通过依赖于Akt和mTORC2活性的PI3K/Akt/mTOR途径诱导自噬,从而减轻炎症对椎间盘细胞的不良影响。因此,我们的发现确定自噬、雷帕霉素和PI3K/Akt/mTOR信号传导是IDD治疗的潜在治疗靶点。
Zotero 插件