Circulating Chromosome Conformation Signatures Significantly Enhance PSA Positive Predicting Value and Overall Accuracy for Prostate Cancer Detection

Author:

Pchejetski Dmitri1ORCID,Hunter Ewan2,Dezfouli Mehrnoush2,Salter Matthew2,Powell Ryan2,Green Jayne2,Naithani Tarun2,Koutsothanasi Christina2ORCID,Alshaker Heba1,Jaipuria Jiten34ORCID,Connor Martin3ORCID,Eldred-Evans David3,Fiorentino Francesca35ORCID,Ahmed Hashim3ORCID,Akoulitchev Alexandre2,Winkler Mathias3

Affiliation:

1. School of Medicine, University of East Anglia, Norwich NR4 7TJ, UK

2. Oxford BioDynamics Limited, Oxford OX4 2WB, UK

3. Department of Surgery and Cancer, Imperial College London, London SW7 2AZ, UK

4. Department of Biotechnology, Amity University, Noida 201313, India

5. Nightingale-Saunders Clinical Trials and Epidemiology Unit, King’s College London, London WC2R 2LS, UK

Abstract

Background: Prostate cancer (PCa) has a high lifetime prevalence (one out of six men), but currently there is no widely accepted screening programme. Widely used prostate specific antigen (PSA) test at cut-off of 3.0 ng/mL does not have sufficient accuracy for detection of any prostate cancer, resulting in numerous unnecessary prostate biopsies in men with benign disease and false reassurance in some men with PCa. We have recently identified circulating chromosome conformation signatures (CCSs, Episwitch® PCa test) allowing PCa detection and risk stratification in line with standards of clinical PCa staging. The purpose of this study was to determine whether combining the Episwitch PCa test with the PSA test will increase its diagnostic accuracy. Methods: n = 109 whole blood samples of men enrolled in the PROSTAGRAM screening pilot study and n = 38 samples of patients with established PCa diagnosis and cancer-negative controls from Imperial College NHS Trust were used. Samples were tested for PSA, and the presence of CCSs in the loci encoding for of DAPK1, HSD3B2, SRD5A3, MMP1, and miRNA98 associated with high-risk PCa identified in our previous work. Results: PSA > 3 ng/mL alone showed a low positive predicted value (PPV) of 0.14 and a high negative predicted value (NPV) of 0.93. EpiSwitch alone showed a PPV of 0.91 and a NPV of 0.32. Combining PSA and Episwitch tests has significantly increased the PPV to 0.81 although reducing the NPV to 0.78. Furthermore, integrating PSA, as a continuous variable (rather than a dichotomised 3 ng/mL cut-off), with EpiSwitch in a new multivariant stratification model, Prostate Screening EpiSwitch (PSE) test, has yielded a remarkable combined PPV of 0.93 and NPV of 0.95 when tested on the independent combined cohort. Conclusions: Our results demonstrate that combining the standard PSA readout with circulating chromosome conformations (PSE test) allows for significantly enhanced PSA PPV and overall accuracy for PCa detection. The PSE test is accurate, rapid, minimally invasive, and inexpensive, suggesting significant screening diagnostic potential to minimise unnecessary referrals for expensive and invasive MRI and/or biopsy testing. Further extended prospective blinded validation of the new combined signature in a screening cohort with low cancer prevalence would be the recommended step for PSE adoption in PCa screening.

Funder

Oxford Biodynamics

Publisher

MDPI AG

Subject

Cancer Research,Oncology

Reference35 articles.

1. ACS (2022, October 01). American Cancer Society. Available online: http://www.cancer.org/cancer/prostatecancer/overviewguide/prostate-cancer-overview-key-statistics.

2. CRUK (2022, October 01). Cancer Research UK. Available online: http://www.cancerresearchuk.org/home/.

3. The Frequency of Carcinoma and Intraepithelial Neoplasia of the Prostate in Young Male Patients;Sakr;J. Urol.,1993

4. Prevalence of PCa and prostatic intraepithelial neoplasia in Caucasian Mediterranean males: An autopsy study;Olmedilla;Prostate,2003

5. The 2016 WHO Classification of Tumours of the Urinary System and Male Genital Organs—Part B: Prostate and Bladder Tumours;Humphrey;Eur. Urol.,2016

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