C-FOS inhibition promotes pancreatic cancer cell ferroptosis by transcriptionally regulating the expression of SLC7A11

IF 3.9 4区 生物学 Q1 GENETICS & HEREDITY Functional & Integrative Genomics Pub Date : 2024-09-18 DOI:10.1007/s10142-024-01429-5
Shuangjia Wang, Hao Yu, Ping Guo, Liuxing Feng, Zhimin Li
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Abstract

Cellular proto-oncogene C-Fos forms the AP-1 transcription factor by dimerizing with proto-oncogene c-Jun; this factor upregulates the transcription of genes associated with different malignancies. However, its functions in pancreatic adenocarcinoma (PAAD) remain poorly understood. In this study, the c-Fos was increased in PAAD cells and tissues through bioinformatic analysis, RT-PCR, and WB. In two PAAD cell lines, PANC-1 and BxPC-3, we performed c-Fos knockdown studies using short hairpin RNA (shRNA). Functional analysis indicated that c-Fos depletion in PAAD cells inhibits cell proliferation and promotes ferroptosis. Chromatin Immunoprecipitation (ChIP) and Dual-luciferase experiments showed that c-Fos coupled to the promoter region of SLC7A11 stimulated its transcription, providing mechanistic insight into the process. Moreover, SLC7A11 blocked the decline of proliferation and ferroptosis by c-Fos knockdown in PAAD cells. Furthermore, a xenograft nude mouse model was established to study the impact of c-Fos on tumorigenesis in vivo. Depletion of c-Fos could suppress PC tumor growth and the expressions of SLC7A11, ki-67, and 4HNE, but overexpression of SLC7A11 reversed this process. In summary, our investigation has shown that c-Fos acts as a transcriptional regulator of SLC7A11, which may enhance tumour growth in pancreatic cancer by inhibiting ferroptosis. These results indicate that c-Fos might be a promising target for treating ferroptosis in PAAD.

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抑制 C-FOS 可通过转录调节 SLC7A11 的表达促进胰腺癌细胞的铁变态反应
细胞原癌基因 C-Fos 通过与原癌基因 c-Jun 二聚形成 AP-1 转录因子;该因子可上调与不同恶性肿瘤相关的基因转录。然而,它在胰腺腺癌(PAAD)中的功能仍鲜为人知。在本研究中,通过生物信息分析、RT-PCR 和 WB,c-Fos 在 PAAD 细胞和组织中增加。在两个 PAAD 细胞系 PANC-1 和 BxPC-3 中,我们使用短发夹 RNA(shRNA)进行了 c-Fos 基因敲除研究。功能分析表明,PAAD 细胞中 c-Fos 的耗竭会抑制细胞增殖并促进铁变态反应。染色质免疫沉淀(ChIP)和双荧光素酶(Dual-luciferase)实验表明,c-Fos与SLC7A11的启动子区域偶联,刺激了SLC7A11的转录,为这一过程提供了机制上的启示。此外,SLC7A11还能阻止PAAD细胞因c-Fos敲除而出现的增殖和铁变态反应。此外,为了研究c-Fos对体内肿瘤发生的影响,我们建立了一个异种移植裸鼠模型。消耗c-Fos可抑制PC肿瘤的生长以及SLC7A11、ki-67和4HNE的表达,但过表达SLC7A11可逆转这一过程。总之,我们的研究表明,c-Fos 是 SLC7A11 的转录调节因子,它可能通过抑制铁突变促进胰腺癌肿瘤的生长。这些结果表明,c-Fos 可能是治疗 PAAD 中铁细胞减少症的一个有前景的靶点。
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来源期刊
CiteScore
3.50
自引率
3.40%
发文量
92
审稿时长
2 months
期刊介绍: Functional & Integrative Genomics is devoted to large-scale studies of genomes and their functions, including systems analyses of biological processes. The journal will provide the research community an integrated platform where researchers can share, review and discuss their findings on important biological questions that will ultimately enable us to answer the fundamental question: How do genomes work?
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