| Literature DB >> 22868251 |
Erica Gianazza1, Clizia Chinello, Veronica Mainini, Marta Cazzaniga, Valeria Squeo, Giancarlo Albo, Stefano Signorini, Salvatore S Di Pierro, Stefano Ferrero, Simone Nicolardi, Yuri E M van der Burgt, André M Deelder, Fulvio Magni.
Abstract
Renal cell carcinoma (RCC) is typically asymptomatic and surgery usually increases patient's life only for early stage tumors. However, some cystic and solid renal lesions cannot be confidently differentiated from clear-cell-RCC. Therefore possible markers for early detection and to distinguish malignant kidney tumors are needed. To this aim, we applied MALDI-TOF and LC-MS/MS analysis to RPC18 MB purified serum of ccRCC, non-ccRCC patients and controls. A cluster of five signals differentiate malignant tumors from benign renal masses and healthy subjects. Moreover, a combination of six ions showed the highest specificity and sensitivity to distinguish ccRCC from controls. Healthy subjects were also differentiated from non-ccRCC by three features. Peptide ratios obtained by MALDI-TOF were compared with those from label-free LC-ESI and no statistical difference was found (p>0.05). ESI-results were linked with MALDI profiles by both TOF/TOF sequencing and MALDI FT-ICR accurate mass measurements. About 200 unique endogenous peptides, originating from 32 proteins, were identified. Among them, SDPR and ZYX were found down-expressed, while SRGN and TMSL3 were up-expressed. In conclusion, our results suggest the possibility to discriminate malignant kidney tumors based on a cluster of serum peptides. Moreover, label-free approach may represent a valid method to verify results obtained by MALDI-TOF. This article is part of a Special Issue entitled: Integrated omics.Entities:
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Year: 2012 PMID: 22868251 DOI: 10.1016/j.jprot.2012.07.032
Source DB: PubMed Journal: J Proteomics ISSN: 1874-3919 Impact factor: 4.044