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使用福尔马林固定石蜡包埋组织的高通量蛋白质组学分析口腔癌中的分子改变

Molecular alterations in oral cancer using high-throughput proteomic analysis of formalin-fixed paraffin-embedded tissue.

作者信息

Mohanty Varshasnata, Subbannayya Yashwanth, Patil Shankargouda, Puttamallesh Vinuth N, Najar Mohd Altaf, Datta Keshava K, Pinto Sneha M, Begum Sameera, Mohanty Neeta, Routray Samapika, Abdulla Riaz, Ray Jay Gopal, Sidransky David, Gowda Harsha, Prasad T S Keshava, Chatterjee Aditi

机构信息

Center for Systems Biology and Molecular Medicine, Yenepoya Research Centre, Yenepoya (Deemed To Be University), Mangalore, Karnataka, 575018, India.

Centre of Molecular Inflammation Research (CEMIR), and Department of Clinical and Molecular Medicine (IKOM), Norwegian University of Science and Technology, N-7491, Trondheim, Norway.

出版信息

J Cell Commun Signal. 2021 Sep;15(3):447-459. doi: 10.1007/s12079-021-00609-3. Epub 2021 Mar 8.

Abstract

Loss of cell differentiation is a hallmark for the progression of oral squamous cell carcinoma (OSCC). Archival Formalin-Fixed Paraffin-Embedded (FFPE) tissues constitute a valuable resource for studying the differentiation of OSCC and can offer valuable insights into the process of tumor progression. In the current study, we performed LC-MS/MS-based quantitative proteomics of FFPE specimens from pathologically-confirmed well-differentiated, moderately-differentiated, and poorly-differentiated OSCC cases. The data were analyzed in four technical replicates, resulting in the identification of 2376 proteins. Of these, 141 and 109 were differentially expressed in moderately-differentiated and poorly differentiated OSCC cases, respectively, compared to well-differentiated OSCC. The data revealed significant metabolic reprogramming with respect to lipid metabolism and glycolysis with proteins belonging to both these processes downregulated in moderately-differentiated OSCC when compared to well-differentiated OSCC. Signaling pathway analysis indicated the alteration of extracellular matrix organization, muscle contraction, and glucose metabolism pathways across tumor grades. The extracellular matrix organization pathway was upregulated in moderately-differentiated OSCC and downregulated in poorly differentiated OSCC, compared to well-differentiated OSCC. PADI4, an epigenetic enzyme transcriptional regulator, and its transcriptional target HIST1H1B were both found to be upregulated in moderately differentiated and poorly differentiated OSCC, indicating epigenetic events underlying tumor differentiation. In conclusion, the findings support the advantage of using high-resolution mass spectrometry-based FFPE archival blocks for clinical and translational research. The candidate signaling pathways identified in the study could be used to develop potential therapeutic targets for OSCC.

摘要

细胞分化丧失是口腔鳞状细胞癌(OSCC)进展的一个标志。存档的福尔马林固定石蜡包埋(FFPE)组织是研究OSCC分化的宝贵资源,可为肿瘤进展过程提供有价值的见解。在本研究中,我们对病理确诊的高分化、中分化和低分化OSCC病例的FFPE标本进行了基于液相色谱-串联质谱(LC-MS/MS)的定量蛋白质组学分析。数据进行了四次技术重复分析,共鉴定出2376种蛋白质。其中,与高分化OSCC相比,分别有141种和109种蛋白质在中分化和低分化OSCC病例中差异表达。数据显示,与高分化OSCC相比,中分化OSCC中参与脂质代谢和糖酵解的蛋白质均下调,表明存在显著的代谢重编程。信号通路分析表明,不同肿瘤分级的细胞外基质组织、肌肉收缩和葡萄糖代谢通路发生改变。与高分化OSCC相比,细胞外基质组织通路在中分化OSCC中上调,在低分化OSCC中下调。表观遗传酶转录调节因子PADI4及其转录靶点HIST1H1B在中分化和低分化OSCC中均上调,表明肿瘤分化存在表观遗传事件。总之,这些发现支持了使用基于高分辨率质谱的FFPE存档样本进行临床和转化研究的优势。本研究中鉴定出的候选信号通路可用于开发OSCC的潜在治疗靶点。

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