Nitric oxide facilitates the S-nitrosylation and deubiquitination of Notch1 protein to maintain cancer stem cells in human NSCLC

IF 5.3
Tenglong Zhang, Jiaxin Lei, Ming Zheng, Zhenke Wen, Juying Zhou
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引用次数: 0

Abstract

Non-small cell lung cancer (NSCLC) is the leading cause of cancer-related mortality, with tumour heterogeneity, fueled by cancer stem cells (CSCs), intricately linked to treatment resistance. Therefore, it is imperative to advance therapeutic strategies targeting CSCs in NSCLC. In this study, we utilized RNA sequencing to investigate metabolic pathway alterations in NSCLC CSCs and identified a crucial role of nitric oxide (NO) metabolism in governing CSC stemness, primarily through modulation of the Notch1 protein. Mechanistically, NO-induced S-nitrosylation of Notch1 facilitated its interaction with the deubiquitylase UCHL1, leading to increased Notch1 protein stability and enhanced CSC stemness. By inhibiting NO synthesis and downregulating UCHL1 expression, we validated the impact of NO on the Notch signalling pathway and CSC stemness. Importantly, targeting NO effectively reduced CSC populations within patient-derived organoids (PDOs) during radiotherapy. This mechanism presents a promising therapeutic target to surmount radiotherapy resistance in NSCLC treatment.

Abstract Image

一氧化氮促进 Notch1 蛋白的 S-亚硝基化和脱泛素化,以维持人类 NSCLC 中的癌症干细胞。
非小细胞肺癌(NSCLC)是导致癌症相关死亡的主要原因,由癌症干细胞(CSCs)引发的肿瘤异质性与耐药性密切相关。因此,推进针对 NSCLC 癌症干细胞的治疗策略势在必行。在这项研究中,我们利用RNA测序技术研究了NSCLC CSCs的代谢途径改变,发现一氧化氮(NO)代谢主要通过调控Notch1蛋白在调控CSC干性方面发挥着关键作用。从机理上讲,NO诱导的Notch1的S-亚硝基化促进了它与去泛素化酶UCHL1的相互作用,从而导致Notch1蛋白稳定性的增加和CSC干性的增强。通过抑制NO的合成和下调UCHL1的表达,我们验证了NO对Notch信号通路和CSC干性的影响。重要的是,在放疗过程中,以NO为靶点可有效减少患者衍生器官组织(PDOs)中的CSC数量。这一机制为克服NSCLC治疗中的放疗耐药性提供了一个很有前景的治疗靶点。
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来源期刊
CiteScore
11.50
自引率
0.00%
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期刊介绍: The Journal of Cellular and Molecular Medicine serves as a bridge between physiology and cellular medicine, as well as molecular biology and molecular therapeutics. With a 20-year history, the journal adopts an interdisciplinary approach to showcase innovative discoveries. It publishes research aimed at advancing the collective understanding of the cellular and molecular mechanisms underlying diseases. The journal emphasizes translational studies that translate this knowledge into therapeutic strategies. Being fully open access, the journal is accessible to all readers.
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