Abstract

IntroductionIntracerebral hemorrhage (ICH) at high altitude is not well understood to date. This study investigates the effects of high altitude on ICH, and examines the acute neuroprotection of hyperbaric oxygen (HBO) therapy against high-altitude ICH.MethodsMinipigs were placed in a hypobaric chamber for 72 h before the operation. ICH was induced by an infusion of autologous arterial blood (3 ml) into the right basal ganglia. Animals in the high-altitude ICH group received HBO therapy (2.5 ATA for 60 min) 30 min after ICH. Blood gas, blood glucose and brain tissue oxygen partial pressure (PbtO2) were monitored continuously for animals from all groups, as were microdialysis products including glucose, lactate, pyruvate and glutamate in perihematomal tissue from 3 to 12 h post-ICH.ResultsHigh-altitude ICH animals showed significantly lower PbtO2, higher lactate/pyruvate ratio (LPR) and glutamate levels than low-altitude ICH animals. More severe neurological deficits, brain edema and neuronal damage were also observed in high-altitude ICH. After HBO therapy, PbtO2 was significantly increased and LPR and glutamate levels were significantly decreased. Brain edema, neurological deficits and neuronal damage were also ameliorated.ConclusionsThe data suggested a more serious disturbance of tissue oxygenation and cerebral metabolism in the acute stage after ICH at high altitude. Early HBO treatment reduced acute brain injury, perhaps through a mechanism involving the amelioration of the derangement of cerebral oxygenation and metabolism following high-altitude ICH.

Highlights

  • Intracerebral hemorrhage (ICH) at high altitude is not well understood to date

  • We know little about secondary brain injury and the pathophysiology related to high-altitude ICH; effective therapy for this disease is very limited

  • There were no significant differences between the plain blood infusion group (PI) and high altitude blood infusion group (HI)-hyperbaric oxygen (HBO) animals at any time point

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Summary

Introduction

Intracerebral hemorrhage (ICH) at high altitude is not well understood to date. Intracerebral hemorrhage (ICH) is the second most common and the deadliest subtype of stroke, with a high mortality rate [1]. It represents between 10 and 15 % of all strokes that occur in the US, Europe and Australia, and between 20 and 30 % of all strokes that occur in Asian countries [2]. We know little about secondary brain injury and the pathophysiology related to high-altitude ICH; effective therapy for this disease is very limited

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