Hypoxia-induced BAP1 enhances erastin-induced ferroptosis in nasopharyngeal carcinoma by stabilizing H2A.

IF 5.3 2区医学 Q1 ONCOLOGY

Cancer Cell International Pub Date : 2024-09-08 DOI:10.1186/s12935-024-03494-z

Weisong Cai, Sa Wu, Zehua Lin, Xiaoping Ming, Xiuping Yang, Minlan Yang, Xiong Chen

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引用次数: 0

Abstract

Background: Hypoxia plays an important role in the chemotherapy resistance of nasopharyngeal carcinoma (NPC). Ferroptosis is a newly discovered form of programmed cell death and ferroptosis inducers showed promising therapeutic effects in some cancers. However, the sensibility of NPC cells to ferroptosis under the hypoxic microenvironment is still unclear, and this study was designed to clarify it.

Methods: NPC cells, treated with erastin, were placed in a normoxia or hypoxic environment (5% CO₂, 94% N₂ and 1% O₂) at 37℃for 24 h. After exposed to hypoxia, ferroptosis-associated phenotypes were detected by CCK8, MDA, GSH, lipid ROS and Fe. The gene expression profiles of head and neck squamous cell carcinoma (HNSCC) tissues were downloaded from the TCGA database to screen construction molecule. BAP1 was screened out and its functions on erastin-induced ferroptosis in NPC cells were detected by knockdown of BAP1. Luciferase reporter assay and co-IP experiment were performed to explore the molecular mechanism. Finally, the tumour xenograft model was applied to further verify these results in vivo.

Results: CCK8 assay showed that IC₅₀ of NPC cells treated with erastin under hypoxia was significantly lower than that under normoxia. Hypoxia significantly increased the levels of lipid ROS and MDA, and decreased GSH content induced by erastin. A prognostic risk model for HNSCC with six ferroptosis-related genes was constructed and validated based on TCGA database. BAP1 was significantly up-regulated under hypoxia, and luciferase reporter assay showed that HIF-1α was an upstream transcription regulator of BAP1. Knockdown of BAP1 in NPC cells significantly increased the IC₅₀ value of erastin under hypoxia and significantly ameliorated erastin-induced ferroptosis under hypoxia in aspect of lipid ROS, MDA content and GSH. Co-IP results showed that BAP1 mediated deubiquitination of H2A and decreased SLC7A11 expression. Finally, knockdown of BAP1 reduced sensitivity to erastin-induced ferroptosis in a tumour xenograft model. And the level of H2A was significantly decreased in xenograft tumors of BAP1 knockdown cells.

Conclusion: Hypoxia-induced BAP1 enhances erastin-induced ferroptosis in NPC by stabilizing H2A. Ferroptosis inducers targeting BAP1 may be an effective way to improve chemotherapy resistance in NPC, especially in the hypoxic microenvironment.

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缺氧诱导的 BAP1 可通过稳定 H2A 增强依拉斯汀诱导的鼻咽癌铁突变。

背景：缺氧在鼻咽癌（NPC）的化疗耐药性中起着重要作用。铁突变是一种新发现的细胞程序性死亡形式，铁突变诱导剂在一些癌症中显示出良好的治疗效果。然而，NPC细胞在缺氧微环境下对铁突变的敏感性仍不清楚，本研究旨在澄清这一点：将经依拉斯汀处理的鼻咽癌细胞置于37℃的常氧或缺氧环境（5% CO2、94% N2和1% O2）中24小时。从 TCGA 数据库下载了头颈部鳞状细胞癌（HNSCC）组织的基因表达谱，以筛选构建分子。筛选出了 BAP1，并通过敲除 BAP1 检测了其在麦拉宁诱导的鼻咽癌细胞铁突变中的功能。通过荧光素酶报告实验和co-IP实验来探索其分子机制。最后，应用肿瘤异种移植模型在体内进一步验证了这些结果：结果：CCK8测定显示，在缺氧条件下，用依拉斯汀处理的鼻咽癌细胞的IC50明显低于正常缺氧条件下的IC50。结果：CCK8测定显示，缺氧条件下，厄拉斯汀处理的鼻咽癌细胞的IC50明显低于正常缺氧条件下的IC50。基于TCGA数据库，构建并验证了包含6个铁蛋白沉积相关基因的HNSCC预后风险模型。BAP1在缺氧条件下明显上调，荧光素酶报告实验表明HIF-1α是BAP1的上游转录调控因子。在鼻咽癌细胞中敲除 BAP1 能明显提高厄拉斯汀在缺氧条件下的 IC50 值，并在脂质 ROS、MDA 含量和 GSH 方面明显改善厄拉斯汀在缺氧条件下诱导的铁变态反应。Co-IP 结果显示，BAP1 介导了 H2A 的去泛素化，并降低了 SLC7A11 的表达。最后，在肿瘤异种移植模型中，敲除 BAP1 可降低对厄拉斯汀诱导的铁变态反应的敏感性。结论：缺氧诱导的BAP1在肿瘤异种移植模型中降低了对依拉斯汀诱导的铁突变的敏感性：缺氧诱导的BAP1通过稳定H2A增强了厄拉斯汀诱导的鼻咽癌铁变态反应。

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

Cancer Cell International ONCOLOGY-

CiteScore

10.90

自引率

1.70%

发文量

360

审稿时长

1 months

期刊介绍： Cancer Cell International publishes articles on all aspects of cancer cell biology, originating largely from, but not limited to, work using cell culture techniques. The journal focuses on novel cancer studies reporting data from biological experiments performed on cells grown in vitro, in two- or three-dimensional systems, and/or in vivo (animal experiments). These types of experiments have provided crucial data in many fields, from cell proliferation and transformation, to epithelial-mesenchymal interaction, to apoptosis, and host immune response to tumors. Cancer Cell International also considers articles that focus on novel technologies or novel pathways in molecular analysis and on epidemiological studies that may affect patient care, as well as articles reporting translational cancer research studies where in vitro discoveries are bridged to the clinic. As such, the journal is interested in laboratory and animal studies reporting on novel biomarkers of tumor progression and response to therapy and on their applicability to human cancers.