Sam68 promotes osteogenic differentiation of aortic valvular interstitial cells by TNF-α/STAT3/autophagy axis

IF 3.6 3区 生物学 Q3 CELL BIOLOGY Journal of Cell Communication and Signaling Pub Date : 2023-02-27 DOI:10.1007/s12079-023-00733-2
Xing Liu, Qiang Zheng, Kan Wang, Jinjing Luo, Zhijie Wang, Huadong Li, Zongtao Liu, Nianguo Dong, Jiawei Shi
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Abstract

Calcified aortic valve disease (CAVD) is a major non-rheumatic heart valve disease in the world, with a high mortality rate and without suitable pharmaceutical therapy due to its complex mechanisms. Src-associated in mitosis 68-KD (Sam68), an RNA binding protein, has been reported as a signaling adaptor in numerous signaling pathways (Huot in Mol Cell Biol, 29(7), 1933-1943, 2009), particularly in inflammatory signaling pathways. The effects of Sam68 on the osteogenic differentiation process of hVICs and its regulation on signal transducer and activator of transcription 3 (STAT3) signaling pathway have been investigated in this study. Human aortic valve samples detection found that Sam68 expression was up-regulated in human calcific aortic valves. We used tumor necrosis factor α (TNF-α) as an activator for osteogenic differentiation in vitro and the result indicated that Sam68 was highly expressed after TNF-α stimulation. Overexpression of Sam68 promoted osteogenic differentiation of hVICs while Sam68 knockdown reversed this effect. Sam68 interaction with STAT3 was predicted by using String database and was verified in this study. Sam68 knockdown reduced phosphorylation of STAT3 activated by TNF-α and the downstream gene expression, which further influenced autophagy flux in hVICs. STAT3 knockdown alleviated the osteogenic differentiation and calcium deposition promoted by Sam68 overexpression. In conclusion, Sam68 interacts with STAT3 and participates in its phosphorylation to promote osteogenic differentiation of hVICs to induce valve calcification. Thus, Sam68 may be a new therapeutic target for CAVD.

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Sam68通过TNF-α/STAT3/自噬轴促进主动脉瓣间质细胞成骨分化
主动脉瓣钙化病(CAVD)是世界上主要的非风湿性心脏瓣膜病,其发病机制复杂,死亡率高,缺乏合适的药物治疗。有丝分裂中src相关的68-KD (Sam68)是一种RNA结合蛋白,已被报道为许多信号通路中的信号转接器(Huot in Mol Cell Biol, 29(7), 1933-1943, 2009),特别是炎症信号通路。本研究探讨了Sam68对hvic成骨分化过程的影响及其对STAT3信号通路的调控作用。人主动脉瓣样品检测发现,Sam68在人钙化主动脉瓣中表达上调。我们用肿瘤坏死因子α (TNF-α)作为体外成骨分化的激活因子,结果表明TNF-α刺激后Sam68高表达。Sam68的过表达促进了hvic的成骨分化,而Sam68的敲低逆转了这一作用。利用String数据库预测Sam68与STAT3的相互作用,并在本研究中进行验证。Sam68敲低可降低TNF-α激活的STAT3磷酸化及下游基因表达,进一步影响hvic的自噬通量。STAT3敲低可减轻Sam68过表达导致的成骨分化和钙沉积。综上所述,Sam68与STAT3相互作用,参与STAT3磷酸化,促进hvic成骨分化,诱导瓣膜钙化。因此,Sam68可能是治疗CAVD的新靶点。
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来源期刊
CiteScore
6.40
自引率
4.90%
发文量
40
期刊介绍: The Journal of Cell Communication and Signaling provides a forum for fundamental and translational research. In particular, it publishes papers discussing intercellular and intracellular signaling pathways that are particularly important to understand how cells interact with each other and with the surrounding environment, and how cellular behavior contributes to pathological states. JCCS encourages the submission of research manuscripts, timely reviews and short commentaries discussing recent publications, key developments and controversies. Research manuscripts can be published under two different sections : In the Pathology and Translational Research Section (Section Editor Andrew Leask) , manuscripts report original research dealing with celllular aspects of normal and pathological signaling and communication, with a particular interest in translational research. In the Molecular Signaling Section (Section Editor Satoshi Kubota) manuscripts report original signaling research performed at molecular levels with a particular interest in the functions of intracellular and membrane components involved in cell signaling.
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