综合基因组学方法确定了follistatin是头颈部鳞状细胞癌中p63-表皮生长因子受体致癌网络的靶点。

NAR Cancer Pub Date : 2023-07-24 eCollection Date: 2023-09-01 DOI:10.1093/narcan/zcad038
Akinsola Oyelakin, Jennifer Sosa, Kasturi Bala Nayak, Alexandra Glathar, Christian Gluck, Isha Sethi, Maria Tsompana, Norma Nowak, Michael Buck, Rose-Anne Romano, Satrajit Sinha
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引用次数: 0

摘要

尽管许多推测的致癌基因与头颈部鳞状细胞癌(HNSCC)的病因有关,但这些致癌基因及其下游靶点介导肿瘤进展的机制尚未完全阐明。我们进行了一项综合分析,以确定致癌转录因子 p63 的一组关键靶标,这些靶标在从 HNSCC 患者和代表性细胞系模型获得的多个转录组数据集中具有共通性。值得注意的是,我们的分析发现,编码follistatin的FST是p63的一个直接转录靶标,follistatin是一种分泌性糖蛋白,可抑制转化生长因子TGFβ/活素信号通路。此外,我们还发现 FST 的表达也受表皮生长因子受体 EGFR 信号转导的驱动,因此介导了 TGF-β 和 EGFR 通路之间的功能联系。我们通过功能缺失和功能增益研究发现,FST 主要赋予 HNSCC 细胞肿瘤生长和迁移表型。此外,对 HNSCC 患者单细胞 RNA 测序数据的分析揭示了癌细胞是肿瘤微环境中 FST 的主要来源,并揭示了 FST 及其调节因子的表达与免疫浸润之间的相关性。我们建议将 FST 作为患者生存的预后生物标志物,并将其作为介导 p63 对肿瘤及其相关微环境产生广泛影响的令人信服的候选因子。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

An integrated genomic approach identifies follistatin as a target of the p63-epidermal growth factor receptor oncogenic network in head and neck squamous cell carcinoma.

An integrated genomic approach identifies follistatin as a target of the p63-epidermal growth factor receptor oncogenic network in head and neck squamous cell carcinoma.

An integrated genomic approach identifies follistatin as a target of the p63-epidermal growth factor receptor oncogenic network in head and neck squamous cell carcinoma.

An integrated genomic approach identifies follistatin as a target of the p63-epidermal growth factor receptor oncogenic network in head and neck squamous cell carcinoma.

Although numerous putative oncogenes have been associated with the etiology of head and neck squamous cell carcinoma (HNSCC), the mechanisms by which these oncogenes and their downstream targets mediate tumor progression have not been fully elucidated. We performed an integrative analysis to identify a crucial set of targets of the oncogenic transcription factor p63 that are common across multiple transcriptomic datasets obtained from HNSCC patients, and representative cell line models. Notably, our analysis revealed FST which encodes follistatin, a secreted glycoprotein that inhibits the transforming growth factor TGFβ/activin signaling pathways, to be a direct transcriptional target of p63. In addition, we found that FST expression is also driven by epidermal growth factor receptor EGFR signaling, thus mediating a functional link between the TGF-β and EGFR pathways. We show through loss- and gain-of-function studies that FST predominantly imparts a tumor-growth and migratory phenotype in HNSCC cells. Furthermore, analysis of single-cell RNA sequencing data from HNSCC patients unveiled cancer cells as the dominant source of FST within the tumor microenvironment and exposed a correlation between the expression of FST and its regulators with immune infiltrates. We propose FST as a prognostic biomarker for patient survival and a compelling candidate mediating the broad effects of p63 on the tumor and its associated microenvironment.

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