Differences in the Volatilomic Urinary Biosignature of Prostate Cancer Patients as a Feasibility Study for the Detection of Potential Biomarkers

Author:

Riccio Giulia12ORCID,Berenguer Cristina V.3ORCID,Perestrelo Rosa3,Pereira Ferdinando4,Berenguer Pedro56ORCID,Ornelas Cristina P.7,Sousa Ana Célia5,Vital João Aragão4,Pinto Maria do Carmo4,Pereira Jorge A. M.3ORCID,Greco Viviana12ORCID,Câmara José S.38ORCID

Affiliation:

1. Department of Basic Biotechnological Sciences, Intensivological and Perioperative Clinics, Univesità Cattolica del Sacro Cuore, 00168 Rome, Italy

2. Unity of Chemistry, Biochemistry and Clinical Molecular Biology, Department of Diagnostic and Laboratory Medicine, Fondazione Policlinico Universitario A. Gemelli IRCCS, 00168 Rome, Italy

3. CQM—Centro de Química da Madeira, NPRG, Universidade da Madeira, Campus da Penteada, 9020-105 Funchal, Portugal

4. Serviço de Urologia, Hospital Dr. Nélio Mendonça, SESARAM, EPERAM—Serviço de Saúde da Região Autónoma da Madeira, Avenida Luís de Camões, nº57, 9004-514 Funchal, Portugal

5. Centro de Investigação Dra Maria Isabel Mendonça, Hospital Dr. Nélio Mendonça, SESARAM, EPERAM, Avenida Luís de Camões, nº57, 9004-514 Funchal, Portugal

6. RO-RAM—Registo Oncológico da Região Autónoma da Madeira, Hospital Dr. Nélio Mendonça, SESARAM, EPERAM, Avenida Luís de Camões, nº57, 9004-514 Funchal, Portugal

7. Centro de Saúde do Bom Jesus, SESARAM, EPERAM, Rua das Hortas, nº67, 9050-024 Funchal, Portugal

8. Departamento de Química, Faculdade de Ciências Exatas e Engenharia, Universidade da Madeira, Campus da Penteada, 9020-105 Funchal, Portugal

Abstract

Prostate cancer (PCa) continues to be the second most common malignant tumour and the main cause of oncological death in men. Investigating endogenous volatile organic metabolites (VOMs) produced by various metabolic pathways is emerging as a novel, effective, and non-invasive source of information to establish the volatilomic biosignature of PCa. In this study, headspace solid-phase microextraction combined with gas chromatography–mass spectrometry (HS-SPME/GC-MS) was used to establish the urine volatilomic profile of PCa and identify VOMs that can discriminate between the two investigated groups. This non-invasive approach was applied to oncological patients (PCa group, n = 26) and cancer-free individuals (control group, n = 30), retrieving a total of 147 VOMs from various chemical families. This included terpenes, norisoprenoid, sesquiterpenes, phenolic, sulphur and furanic compounds, ketones, alcohols, esters, aldehydes, carboxylic acid, benzene and naphthalene derivatives, hydrocarbons, and heterocyclic hydrocarbons. The data matrix was subjected to multivariate analysis, namely partial least-squares discriminant analysis (PLS-DA). Accordingly, this analysis showed that the group under study presented different volatomic profiles and suggested potential PCa biomarkers. Nevertheless, a larger cohort of samples is required to boost the predictability and accuracy of the statistical models developed.

Funder

FCT-Fundação para a Ciência e a Tecnologia

ARDITI-Agência Regional para o Desenvolvimento da Investigação Tecnologia e Inovação

Univesità Cattolica del Sacro Cuore

ARDITI

Núcleo Regional da Madeira da Liga Portuguesa contra o Cancro

Bolsa Rubina Barros

Fundação para a Ciência e Tecnologia and Madeira

Publisher

MDPI AG

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