1. In-Depth Mapping of the Urinary N-Glycoproteome: Distinct Signatures of ccRCC-related Progression
- Author
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Marco Grasso, Isabella Piga, Francesca Raimondo, Francesca Clerici, Vanna Denti, Clizia Chinello, Giulia Capitoli, Angelica Grasso, Fulvio Magni, Andrew Smith, Lucia Santorelli, Santorelli, L, Capitoli, G, Chinello, C, Piga, I, Clerici, F, Denti, V, Smith, A, Grasso, A, Raimondo, F, Grasso, M, and Magni, F
- Subjects
Cancer Research ,Glycosylation ,Apolipoprotein B ,Glycoproteomic ,Urinary system ,N-glycomapping ,Urine ,lcsh:RC254-282 ,Article ,chemistry.chemical_compound ,glycoproteomics ,Medicine ,Stage (cooking) ,biology ,business.industry ,Clear cell Renal Cell Carcinoma ,Translation (biology) ,lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens ,medicine.disease ,Glycoproteomics ,Clear cell renal cell carcinoma ,Oncology ,chemistry ,biology.protein ,Cancer research ,Label-free ,business ,Glycomarker ,Kidney cancer ,glycomarkers - Abstract
Protein N-glycosylation is one of the most important post-translational modifications and is involved in many biological processes, with aberrant changes in protein N-glycosylation patterns being closely associated with several diseases, including the progression and spreading of tumours. In light of this, identifying these aberrant protein glycoforms in tumours could be useful for understanding the molecular mechanism of this multifactorial disease, developing specific biomarkers and finding novel therapeutic targets. We investigated the urinary N-glycoproteome of clear cell renal cell carcinoma (ccRCC) patients at different stages (n = 15 at pT1 and n = 15 at pT3), and of non-ccRCC subjects (n = 15), using an N-glyco-FASP-based method. Using label-free nLC-ESI MS/MS, we identified and quantified several N-glycoproteins with altered expression and abnormal changes affecting the occupancy of the glycosylation site in the urine of RCC patients compared to control. In particular, nine of them had a specific trend that was directly related to the stage progression: CD97, COCH and P3IP1 were up-expressed whilst APOB, FINC, CERU, CFAH, HPT and PLTP were down-expressed in ccRCC patients. Overall, these results expand our knowledge related to the role of this post-translational modification in ccRCC and translation of this information into pre-clinical studies could have a significant impact on the discovery of novel biomarkers and therapeutic target in kidney cancer.
- Published
- 2020
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