Large-scale and high-resolution mass spectrometry-based proteomics profiling defines molecular subtypes of esophageal cancer for therapeutic targeting.
Wei LiuLei XieYao-Hui HeZhi-Yong WuLu-Xin LiuXue-Feng BaiDan-Xia DengXiu-E XuLian-Di LiaoWan LinJing-Hua HengXin XuLiu PengQing-Feng HuangCheng-Yu LiZhi-Da ZhangWei WangGuo-Rui ZhangXiang GaoShao-Hong WangChun-Quan LiLi-Yan XuWen LiuEn-Min LiPublished in: Nature communications (2021)
Esophageal cancer (EC) is a type of aggressive cancer without clinically relevant molecular subtypes, hindering the development of effective strategies for treatment. To define molecular subtypes of EC, we perform mass spectrometry-based proteomic and phosphoproteomics profiling of EC tumors and adjacent non-tumor tissues, revealing a catalog of proteins and phosphosites that are dysregulated in ECs. The EC cohort is stratified into two molecular subtypes-S1 and S2-based on proteomic analysis, with the S2 subtype characterized by the upregulation of spliceosomal and ribosomal proteins, and being more aggressive. Moreover, we identify a subtype signature composed of ELOA and SCAF4, and construct a subtype diagnostic and prognostic model. Potential drugs are predicted for treating patients of S2 subtype, and three candidate drugs are validated to inhibit EC. Taken together, our proteomic analysis define molecular subtypes of EC, thus providing a potential therapeutic outlook for improving disease outcomes in patients with EC.
Keyphrases
- mass spectrometry
- liquid chromatography
- high resolution mass spectrometry
- single molecule
- end stage renal disease
- ejection fraction
- cell proliferation
- newly diagnosed
- signaling pathway
- papillary thyroid
- drug delivery
- cancer therapy
- risk assessment
- replacement therapy
- smoking cessation
- prognostic factors
- patient reported
- capillary electrophoresis
- lymph node metastasis
- squamous cell