Lifelong exposure to high‐altitude hypoxia in humans is associated with improved redox homeostasis and structural–functional adaptations of the neurovascular unit

Author:

Stacey Benjamin S.1ORCID,Hoiland Ryan L.23ORCID,Caldwell Hannah G.4ORCID,Howe Connor A.4ORCID,Vermeulen Tyler4ORCID,Tymko Michael M.456,Vizcardo‐Galindo Gustavo A.7ORCID,Bermudez Daniella7ORCID,Figueroa‐Mujíica Rómulo J.7ORCID,Gasho Christopher8,Tuaillon Edouard9,Hirtz Christophe10ORCID,Lehmann Sylvain10,Marchi Nicola11,Tsukamoto Hayato12ORCID,Villafuerte Francisco C.7ORCID,Ainslie Philip N.14ORCID,Bailey Damian M.1ORCID

Affiliation:

1. Neurovascular Research Laboratory, Faculty of Life Sciences and Education University of South Wales Pontypridd UK

2. Department of Anaesthesiology, Pharmacology and Therapeutics, Vancouver General Hospital University of British Columbia Vancouver British Columbia Canada

3. Department of Cellular and Physiological Sciences, Faculty of Medicine University of British Columbia Vancouver British Columbia Canada

4. Centre for Heart, Lung and Vascular Health University of British Columbia‐Okanagan Campus Kelowna British Columbia Canada

5. Faculty of Kinesiology, Sport, and Recreation University of Alberta Edmonton Alberta Canada

6. Department of Medicine, Faculty of Medicine University of British Columbia Vancouver British Columbia Canada

7. Laboratorio de Fisiología Comparada, Departamento de Ciencias Biológicas y Fisiológicas, Facultad de Ciencias y Filosofía Universidad Peruana Cayetano Heredia Lima 31 Peru

8. Division of Pulmonary and Critical Care Loma Linda University School of Medicine Loma Linda CA USA

9. Department of Infectious Diseases University of Montpellier Montpellier France

10. LBPC‐PPC Université de Montpellier, IRMB CHU de Montpellier, INM INSERM Montpellier France

11. Laboratory of Cerebrovascular and Glia Research, Department of Neuroscience, Institute of Functional Genomics University of Montpellier Montpellier France

12. Faculty of Sport and Health Science Ritsumeikan University Kusatsu Shiga Japan

Abstract

AbstractHigh‐altitude (HA) hypoxia may alter the structural–functional integrity of the neurovascular unit (NVU). Herein, we compared male lowlanders (n = 9) at sea level (SL) and after 14 days acclimatization to 4300 m (chronic HA) in Cerro de Pasco (CdP), Péru (HA), against sex‐, age‐ and body mass index‐matched healthy highlanders (n = 9) native to CdP (lifelong HA). Venous blood was assayed for serum proteins reflecting NVU integrity, in addition to free radicals and nitric oxide (NO). Regional cerebral blood flow (CBF) was examined in conjunction with cerebral substrate delivery, dynamic cerebral autoregulation (dCA), cerebrovascular reactivity to carbon dioxide (CVRCO2) and neurovascular coupling (NVC). Psychomotor tests were employed to examine cognitive function. Compared to lowlanders at SL, highlanders exhibited elevated basal plasma and red blood cell NO bioavailability, improved anterior and posterior dCA, elevated anterior CVRCO2 and preserved cerebral substrate delivery, NVC and cognition. In highlanders, S100B, neurofilament light‐chain (NF‐L) and T‐tau were consistently lower and cognition comparable to lowlanders following chronic‐HA. These findings highlight novel integrated adaptations towards regulation of the NVU in highlanders that may represent a neuroprotective phenotype underpinning successful adaptation to the lifelong stress of HA hypoxia. imageKey points High‐altitude (HA) hypoxia has the potential to alter the structural–functional integrity of the neurovascular unit (NVU) in humans. For the first time, we examined to what extent chronic and lifelong hypoxia impacts multimodal biomarkers reflecting NVU structure and function in lowlanders and native Andean highlanders. Despite lowlanders presenting with a reduction in systemic oxidative–nitrosative stress and maintained cerebral bioenergetics and cerebrovascular function during chronic hypoxia, there was evidence for increased axonal injury and cognitive impairment. Compared to lowlanders at sea level, highlanders exhibited elevated vascular NO bioavailability, improved dynamic regulatory capacity and cerebrovascular reactivity, comparable cerebral substrate delivery and neurovascular coupling, and maintained cognition. Unlike lowlanders following chronic HA, highlanders presented with lower concentrations of S100B, neurofilament light chain and total tau. These findings highlight novel integrated adaptations towards the regulation of the NVU in highlanders that may represent a neuroprotective phenotype underpinning successful adaptation to the lifelong stress of HA hypoxia.

Funder

Higher Education Funding Council for Wales

Wellcome Trust

Publisher

Wiley

Subject

Physiology

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