Profiling of urinary extracellular vesicle protein signatures from patients with cribriform and intraductal prostate carcinoma in a cross-sectional study

Author:

Matthiesen Rune1,Carvalho Ana2,Leão Ricardo3,Sayyid Rashid4,Pereira Hermínia5,Beck Hans6,Bernardino Rui4,Pinheiro Luis7,Henrique Rui8,Fleshner Neil4,Alves Liliana1,Hall Michael1

Affiliation:

1. NOVA Medical School-Research, Faculdade de Ciências Médicas

2. Universidade NOVA de Lisboa,

3. Cuf Hospitais, Lisbon

4. Princess Margaret Cancer Centre

5. Department of Pathology, Centro Hospitalar e Universitário Lisboa Central, Lisbon

6. Centre for Clinical Proteomics, Department of Clinical Biochemistry, Odense University Hospital

7. Department of Urology, Centro Hospitalar e Universitário Lisboa Central, Lisbon

8. Department of Pathology and Molecular Immunology, ICBAS – School of Medicine and Biomedical Sciences, University of Porto (ICBAS-UP)

Abstract

Abstract

Prognostic tests and treatment approaches for optimized clinical care of prostatic neoplasms are an unmet need. Prostate cancer (PCa) and associated extracellular vesicles (EVs) proteome changes occur during initiation and progression of the disease. PCa tissue proteome has been previously characterized, but screening of tissue samples constitutes an invasive procedure. Consequently, we focused this study on liquid biopsies, such as urine samples. More specifically, urinary small extracellular vesicle and particles proteome profiles of 100 subjects were analyzed using liquid chromatography coupled to high-resolution mass spectrometry (LC-MS/MS). We identified 171 proteins that were differentially expressed between intraductal prostate cancer/cribriform (IDC/Crib) and non-IDC/non-Crib after correction for multiple testing. However, the strong correlation between IDC/Crib and Gleason Grade complicates the disentanglement of the underlying factors driving this association. Nevertheless, even after accounting for multiple testing and adjusting for ISUP (International Society of Urological Pathology) grading, two proteins continued to exhibit significant differential expression between IDC/Crib and non-IDC/non-Crib. Functional enrichment analysis based on cancer hallmark proteins disclosed a clear pattern of androgen response down-regulation in urinary EVs from IDC/Crib compared to non-IDC/non-Crib. Interestingly, proteome differences between IDC and cribriform were more subtle, suggesting high proteome heterogeneity. Overall, the urinary EV proteome reflect partly the prostate pathology.

Publisher

Research Square Platform LLC

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