4.7 Article

Pushing arterial-venous plasma biomarkers to new heights: A model for personalised redox metabolomics?

Journal

REDOX BIOLOGY
Volume 21, Issue -, Pages -

Publisher

ELSEVIER
DOI: 10.1016/j.redox.2019.101113

Keywords

Thiols; Altitude; Hypoxia; Oxygen; Oxidative stress; Hydrogen sulfide

Funding

  1. Deltex
  2. Smiths Medical
  3. Amazon Medical
  4. Aurapa GmbH
  5. Bloc Eyewear
  6. Cheetah Medical
  7. Cotswold Outdoor
  8. Deltex Medical
  9. Foam Techniques
  10. Gortons Chartered Accountants
  11. Hutchinson Telecom
  12. Labcold
  13. La Sportiva
  14. Lyon Equipment
  15. PanGas (The Linde Group)
  16. Manbat
  17. Mercedes-Benz
  18. Mountain Equipment
  19. Multimat
  20. Northgate Vehicle Hire
  21. Pangas
  22. PMS Instruments
  23. PO Ferries
  24. Proact Medical
  25. Royal Leisure
  26. Siemens
  27. UCL Provost
  28. Friends of UCLH
  29. UK Medical Research Council [G1001536]
  30. UK Medical Research Council (Strategic Appointment Scheme)
  31. Faculty of Medicine, University of Southampton
  32. Cancer Research UK [C21825/A23904]
  33. NIHR Academic Clinical Fellowship
  34. MRC [G1001536, G0701115] Funding Source: UKRI

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The chemical and functional interactions between Reactive Oxygen (ROS), Nitrogen (RNS) and Sulfur (RSS) species allow organisms to detect and respond to metabolic and environmental stressors, such as exercise and altitude exposure. Whether redox markers and constituents of this 'Reactive Species Interactome' (RSI) differ in concentration between arterial and venous blood is unknown. We hypothesised that such measurements may provide useful insight into metabolic/redox regulation at the whole-body level and would be consistent between individuals exposed to identical challenges. An exploratory study was performed during the Xtreme Alps expedition in 2010 in which four healthy individuals (2 male, 2 female) underwent paired arterial and central venous blood sampling before, during and after performance of a constant-work-rate cardiopulmonary exercise test, at sea level and again at 4559 m. Unexpectedly, plasma total free thiol and free cysteine concentrations remained substantially elevated at altitude throughout exercise with minimal arteriovenous gradients. Free sulfide concentrations changed only modestly upon combined altitude/exercise stress, whereas bound sulfide levels were lower at altitude than sea-level. No consistent signal indicative of the expected increased oxidative stress and nitrate -> nitrite -> NO reduction was observed with 4-hydroxynonenal, isoprostanes, nitrate, nitrite, nitroso species and cylic guanosine monophosphate. However, the observed arteriovenous concentration differences revealed a dynamic pattern of response that was unique to each participant. This novel redox metabolomic approach of obtaining quantifiable 'metabolic signatures' to a defined physiological challenge could potentially offer new avenues for personalised medicine.

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