METTL14 decreases FTH1 mRNA stability via m6A methylation to promote sorafenib-induced ferroptosis of cervical cancer.

IF 5.4 3区 材料科学 Q2 CHEMISTRY, PHYSICAL
ACS Applied Energy Materials Pub Date : 2024-12-31 Epub Date: 2024-05-13 DOI:10.1080/15384047.2024.2349429
Lijie Li, Jie Zeng, Sili He, Yanfei Yang, Chen Wang
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引用次数: 0

Abstract

Cervical cancer (CC) is a prevalent malignancy among women worldwide. This study was designed to investigate the role of METTL14 in sorafenib-induced ferroptosis in CC. METTL14 expression and m6A methylation were determined in CC tissues, followed by analyzes correlating these factors with clinical features. Subsequently, METTL14 was knocked down in CC cell lines, and the effects on cell proliferation, mitochondrial morphology and ferroptosis were assessed using CCK-8, microscopy, and markers associated with ferroptosis, respectively. The regulatory relationship between METTL14 and FTH1 was verified using qRT-PCR and luciferase reporter assays. The functional significance of this interaction was further investigated both in vitro and in vivo by co-transfecting cells with overexpression vectors or shRNAs targeting METTL14 and FTH1 after sorafenib treatment. METTL14 expression and m6A methylation were significantly reduced in CC tissues, and lower METTL14 expression levels were associated with a poorer CC patients' prognosis. Notably, METTL14 expression increased during sorafenib-induced ferroptosis, and METTL14 knockdown attenuated the ferroptotic response induced by sorafenib in CC cells. FTH1 was identified as a direct target of METTL14, with METTL14 overexpression leading to increased m6A methylation of FTH1 mRNA, resulting in reduced stability and expression of FTH1 in CC. Furthermore, FTH1 overexpression or treatment with LY294002 partially counteracted the promotion of sorafenib-induced ferroptosis by METTL14. In vivo xenograft experiments demonstrated that inhibiting METTL14 reduced the anticancer effects of sorafenib, whereas suppression of FTH1 significantly enhanced sorafenib-induced ferroptosis and increased its anticancer efficacy. METTL14 reduces FTH1 mRNA stability through m6A methylation, thereby enhancing sorafenib-induced ferroptosis, which contributes to suppressing CC progression via the PI3K/Akt signaling pathway.

METTL14通过m6A甲基化降低FTH1 mRNA的稳定性,从而促进索拉非尼诱导的宫颈癌铁变态反应。
宫颈癌(CC)是全球妇女中普遍存在的恶性肿瘤。本研究旨在探讨METTL14在索拉非尼诱导的宫颈癌铁中毒中的作用。研究测定了CC组织中METTL14的表达和m6A甲基化,并分析了这些因素与临床特征的相关性。随后,在CC细胞系中敲除METTL14,并使用CCK-8、显微镜和与铁变态相关的标记物分别评估其对细胞增殖、线粒体形态和铁变态的影响。通过 qRT-PCR 和荧光素酶报告实验验证了 METTL14 和 FTH1 之间的调控关系。索拉非尼治疗后,通过过表达载体或靶向 METTL14 和 FTH1 的 shRNAs 共同转染细胞,进一步研究了这种相互作用在体外和体内的功能意义。在CC组织中,METTL14的表达和m6A甲基化明显降低,而较低的METTL14表达水平与CC患者较差的预后有关。值得注意的是,在索拉非尼诱导的铁变态反应过程中,METTL14的表达会增加,而METTL14的敲除会减弱索拉非尼在CC细胞中诱导的铁变态反应。FTH1被确定为METTL14的直接靶标,METTL14过表达会导致FTH1 mRNA的m6A甲基化增加,从而降低FTH1在CC中的稳定性和表达。此外,FTH1过表达或用LY294002治疗可部分抵消METTL14对索拉非尼诱导的铁变态反应的促进作用。体内异种移植实验表明,抑制METTL14会降低索拉非尼的抗癌效果,而抑制FTH1则会显著增强索拉非尼诱导的铁细胞沉降,提高其抗癌疗效。METTL14通过m6A甲基化降低了FTH1 mRNA的稳定性,从而增强了索拉非尼诱导的铁变态反应,这有助于通过PI3K/Akt信号通路抑制CC的进展。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
ACS Applied Energy Materials
ACS Applied Energy Materials Materials Science-Materials Chemistry
CiteScore
10.30
自引率
6.20%
发文量
1368
期刊介绍: ACS Applied Energy Materials is an interdisciplinary journal publishing original research covering all aspects of materials, engineering, chemistry, physics and biology relevant to energy conversion and storage. The journal is devoted to reports of new and original experimental and theoretical research of an applied nature that integrate knowledge in the areas of materials, engineering, physics, bioscience, and chemistry into important energy applications.
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