Zinc stable isotopes in urine as diagnostic for cancer of secretory organs

Author:

Schilling Kathrin1ORCID,Moore Rebekah E T2ORCID,Sullivan Kaj V3ORCID,Capper Miles S2ORCID,Rehkämper Mark2ORCID,Goddard Kate4,Ion Charlotte4,Coombes R Charles4ORCID,Vesty-Edwards Lois5,Lamb Alastair D5ORCID,Halliday Alex N6,Larner Fiona78ORCID

Affiliation:

1. Lamont-Doherty Earth Observatory, Columbia University, Palisades, NY, USA

2. Department of Earth Science and Engineering, Imperial College London, London, UK

3. Department of Renewable Resources, University of Alberta, Alberta, Canada

4. Imperial College Healthcare NHS Trust, London, UK

5. Nuffield Department of Surgical Sciences, University of Oxford, Oxford, UK

6. Earth Institute, Columbia University, New York, NY, USA

7. Department of Earth Sciences, University of Oxford, South Parks Road, Oxford, UK

8. St Catherine's College, University of Oxford, Manor Road, Oxford, UK

Abstract

Abstract Breast, prostate, and pancreatic cancers alter the zinc (Zn) metabolism. Combined analyses of urinary Zn concentrations [Zn] and Zn stable isotope compositions (δ66Zn) may provide a non-invasive approach for tracing malignancy-induced Zn dyshomeostasis. In this study, we measured [Zn] and δ66Zn in urine from prostate (n = 22), breast (n = 16), and from women with benign breast disease (n = 14) and compared those with age-matched healthy controls (22–49 years or 50+ years) and published data for pancreatic cancer (n = 17). Our results show that cancer-induced changes are reflected in higher urinary [Zn] and lower urinary δ66Zn for pancreatic and prostate cancer and benign breast disease when compared with healthy controls. For prostate cancer, the progression of low [Zn] and high δ66Zn for patients of low-risk disease toward high [Zn] and low δ66Zn for the higher risk patients demonstrates that [Zn] and δ66Zn in urine could serve as a reliable prognostic tool. Urinary excretion of isotopically light Zn by patients with prostatic and pancreatic cancer is probably the result of increased reactive oxygen species in cancerous cells, which limits the scavenging of hydroxyl radicals and thus facilitates the oxidation of metalloproteins with sulfur-rich ligands. Urine from breast cancer patients shows undistinguishable δ66Zn to healthy controls, implying that the expression of metalloproteins with sulfur-rich ligands is stronger in breast cancer tissues. In conclusion, urinary δ66Zn may provide a non-invasive diagnostic tool for pancreatic cancer and support disease prognosis for prostate cancer. These findings should translate to comprehensive transverse and longitudinal cohort studies in future.

Funder

National Institute for Health Research Imperial Biomedical Research Centre

Imperial Experimental Cancer Medicine Centre

Cancer Research UK Imperial Centre at Imperial College London

Publisher

Oxford University Press (OUP)

Subject

Metals and Alloys,Biochemistry,Biomaterials,Biophysics,Chemistry (miscellaneous)

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