Vibrational spectroscopy of liquid biopsies for prostate cancer diagnosis

Author:

Medipally Dinesh K. R.12ORCID,Cullen Daniel12,Untereiner Valérie34,Sockalingum Ganesh D.3,Maguire Adrian12,Nguyen Thi Nguyet Que12,Bryant Jane1,Noone Emma5,Bradshaw Shirley5,Finn Marie5,Dunne Mary5,Shannon Aoife M.6,Armstrong John67,Meade Aidan D.81ORCID,Lyng Fiona M92

Affiliation:

1. Radiation and Environmental Science Centre, Focas Research Institute, Technological University Dublin, Dublin, Ireland

2. School of Physics & Clinical & Optometric Sciences, Technological University Dublin, Dublin, Ireland

3. Université de Reims Champagne−Ardenne, BioSpecT EA 7506, UFR Pharmacie, Reims, France

4. Université de Reims Champagne−Ardenne, PICT, Reims, France

5. Clinical Trials Unit, St Luke’s Radiation Oncology Network, St Luke’s Hospital, Dublin, Ireland

6. Cancer Trials Ireland, Dublin, Ireland

7. Department of Radiation Oncology, St Luke’s Radiation Oncology Network, St Luke’s Hospital, Dublin, Ireland

8. School of Physics & Clinical & Optometric Sciences, Technological University Dublin, Kevin Street, Dublin, Dublin D08 NF82, Ireland

9. Radiation and Environmental Science Centre, Focas Research Institute, Technological University Dublin, Dublin, Dublin D08 NF82, Ireland

Abstract

Background: Screening for prostate cancer with prostate specific antigen and digital rectal examination allows early diagnosis of prostate malignancy but has been associated with poor sensitivity and specificity. There is also a considerable risk of over-diagnosis and over-treatment, which highlights the need for better tools for diagnosis of prostate cancer. This study investigates the potential of high throughput Raman and Fourier Transform Infrared (FTIR) spectroscopy of liquid biopsies for rapid and accurate diagnosis of prostate cancer. Methods: Blood samples (plasma and lymphocytes) were obtained from healthy control subjects and prostate cancer patients. FTIR and Raman spectra were recorded from plasma samples, while Raman spectra were recorded from the lymphocytes. The acquired spectral data was analysed with various multivariate statistical methods, principal component analysis (PCA), partial least squares discriminant analysis (PLS-DA) and classical least squares (CLS) fitting analysis. Results: Discrimination was observed between the infrared and Raman spectra of plasma and lymphocytes from healthy donors and prostate cancer patients using PCA. In addition, plasma and lymphocytes displayed differentiating signatures in patients exhibiting different Gleason scores. A PLS-DA model was able to discriminate these groups with sensitivity and specificity rates ranging from 90% to 99%. CLS fitting analysis identified key analytes that are involved in the development and progression of prostate cancer. Conclusions: This technology may have potential as an alternative first stage diagnostic triage for prostate cancer. This technology can be easily adaptable to many other bodily fluids and could be useful for translation of liquid biopsy-based diagnostics into the clinic.

Funder

EU FP7 Network of Excellence DoReMi

Science Foundation Ireland

European Cooperation in Science and Technology

Irish Research Council

Publisher

SAGE Publications

Subject

Oncology

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