Abstract

To screen proteins/peptides in urine of Renal Cell Carcinoma (RCC) patients by SELDI-TOF (Surface Enhanced Laser Desorption Ionization - Time of Flight) in search of possible biomarkers. Sixty-one urines samples from Clear Cell RCC and Papillary RCC were compared to 29 samples of control urine on CM10 chip. Mass analysis was performed in a ProteinChip Reader PCS 4,000 (Ciphergen Biosystems, Fremont, CA) with the software Ciphergen Express 3.0. All chips were read at low and at high laser energy. For statistical analysis the urine samples were clustered according to the histological classification (Clear Cell and Papillary Carcinoma). For identification urine was loaded on a SDS PAGE gel and bands of most interest were excised, trypsinized and identified by MS/MS. Databank searches were performed in Swiss-Prot database using the MASCOT search algorithm and in Profound. Proteins that were identified from urine of controls included immunoglobulin light chains, albumin, secreted and transmembrane 1 precursor (protein K12), mannan-binding lectin-associated serine protease-2 (MASP-2) and vitelline membrane outer layer 1 isoform 1. Identification of immunoglobulins and isoforms of albumin are quite common by proteomics and therefore cannot be considered as possible molecular markers. K12 and MASP-2 play important physiological roles, while vitellite membrane outer layer 1 role is unknown since it was never purified in humans. The down expression of Protein K-12 and MASP-2 make them good candidates for RCC urine marker and should be validated in a bigger cohort including the other less common histological RCC subtypes.

Highlights

  • Urine analysis is a non-invasive method of clinical analysis and has been used primarily to monitor diseases of the urogenital tract

  • Most of them come from the glomerular filtrate of plasma, while others from ibju | Urine screening by Seldi-Tof in patients with Renal Cell Carcinoma the process of apoptosis and the cleavage of membrane proteins that are secreted

  • High molecular weight proteins are able to pass through the glomerular filtrate

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Summary

Introduction

Urine analysis is a non-invasive method of clinical analysis and has been used primarily to monitor diseases of the urogenital tract. Most of them come from the glomerular filtrate of plasma, while others from ibju | Urine screening by Seldi-Tof in patients with Renal Cell Carcinoma the process of apoptosis and the cleavage of membrane proteins that are secreted. High molecular weight proteins (albumin, for example) are able to pass through the glomerular filtrate. Peptides (< 10 kDa) are filtered by the glomerulus and constitute an important source of information, even if the peptide is the result of proteolysis of larger proteins circulating in plasma [1,2,3]. Urine is especially attractive for biomarker discovery in urological diseases since any change in concentration of proteins in plasma will reflect in the urine

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