Cerebral vascular control and metabolism in heat stress

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Cerebral vascular control and metabolism in heat stress. / Bain, Anthony R; Nybo, Lars; Ainslie, Philip N.

I: Comprehensive Physiology, Bind 5, Nr. 3, 2015, s. 1345-1380.

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningfagfællebedømt

Harvard

Bain, AR, Nybo, L & Ainslie, PN 2015, 'Cerebral vascular control and metabolism in heat stress', Comprehensive Physiology, bind 5, nr. 3, s. 1345-1380. https://doi.org/10.1002/cphy.c140066

APA

Bain, A. R., Nybo, L., & Ainslie, P. N. (2015). Cerebral vascular control and metabolism in heat stress. Comprehensive Physiology, 5(3), 1345-1380. https://doi.org/10.1002/cphy.c140066

Vancouver

Bain AR, Nybo L, Ainslie PN. Cerebral vascular control and metabolism in heat stress. Comprehensive Physiology. 2015;5(3):1345-1380. https://doi.org/10.1002/cphy.c140066

Author

Bain, Anthony R ; Nybo, Lars ; Ainslie, Philip N. / Cerebral vascular control and metabolism in heat stress. I: Comprehensive Physiology. 2015 ; Bind 5, Nr. 3. s. 1345-1380.

Bibtex

@article{b80fd82697344a6687b2496799348c3e,
title = "Cerebral vascular control and metabolism in heat stress",
abstract = "This review provides an in-depth update on the impact of heat stress on cerebrovascular functioning. The regulation of cerebral temperature, blood flow, and metabolism are discussed. We further provide an overview of vascular permeability, the neurocognitive changes, and the key clinical implications and pathologies known to confound cerebral functioning during hyperthermia. A reduction in cerebral blood flow (CBF), derived primarily from a respiratory-induced alkalosis, underscores the cerebrovascular changes to hyperthermia. Arterial pressures may also become compromised because of reduced peripheral resistance secondary to skin vasodilatation. Therefore, when hyperthermia is combined with conditions that increase cardiovascular strain, for example, orthostasis or dehydration, the inability to preserve cerebral perfusion pressure further reduces CBF. A reduced cerebral perfusion pressure is in turn the primary mechanism for impaired tolerance to orthostatic challenges. Any reduction in CBF attenuates the brain's convective heat loss, while the hyperthermic-induced increase in metabolic rate increases the cerebral heat gain. This paradoxical uncoupling of CBF to metabolism increases brain temperature, and potentiates a condition whereby cerebral oxygenation may be compromised. With levels of experimentally viable passive hyperthermia (up to 39.5-40.0°C core temperature), the associated reduction in CBF (∼30%) and increase in cerebral metabolic demand (∼10%) is likely compensated by increases in cerebral oxygen extraction. However, severe increases in whole-body and brain temperature may increase blood-brain barrier permeability, potentially leading to cerebral vasogenic edema. The cerebrovascular challenges associated with hyperthermia are of paramount importance for populations with compromised thermoregulatory control-for example, spinal cord injury, elderly, and those with preexisting cardiovascular diseases. {\textcopyright} 2015 American Physiological Society. Compr Physiol 5:1345-1380, 2015.",
author = "Bain, {Anthony R} and Lars Nybo and Ainslie, {Philip N}",
note = "CURIS 2015 NEXS 261",
year = "2015",
doi = "10.1002/cphy.c140066",
language = "English",
volume = "5",
pages = "1345--1380",
journal = "Comprehensive Physiology",
issn = "2040-4603",
publisher = "Wiley-Blackwell",
number = "3",

}

RIS

TY - JOUR

T1 - Cerebral vascular control and metabolism in heat stress

AU - Bain, Anthony R

AU - Nybo, Lars

AU - Ainslie, Philip N

N1 - CURIS 2015 NEXS 261

PY - 2015

Y1 - 2015

N2 - This review provides an in-depth update on the impact of heat stress on cerebrovascular functioning. The regulation of cerebral temperature, blood flow, and metabolism are discussed. We further provide an overview of vascular permeability, the neurocognitive changes, and the key clinical implications and pathologies known to confound cerebral functioning during hyperthermia. A reduction in cerebral blood flow (CBF), derived primarily from a respiratory-induced alkalosis, underscores the cerebrovascular changes to hyperthermia. Arterial pressures may also become compromised because of reduced peripheral resistance secondary to skin vasodilatation. Therefore, when hyperthermia is combined with conditions that increase cardiovascular strain, for example, orthostasis or dehydration, the inability to preserve cerebral perfusion pressure further reduces CBF. A reduced cerebral perfusion pressure is in turn the primary mechanism for impaired tolerance to orthostatic challenges. Any reduction in CBF attenuates the brain's convective heat loss, while the hyperthermic-induced increase in metabolic rate increases the cerebral heat gain. This paradoxical uncoupling of CBF to metabolism increases brain temperature, and potentiates a condition whereby cerebral oxygenation may be compromised. With levels of experimentally viable passive hyperthermia (up to 39.5-40.0°C core temperature), the associated reduction in CBF (∼30%) and increase in cerebral metabolic demand (∼10%) is likely compensated by increases in cerebral oxygen extraction. However, severe increases in whole-body and brain temperature may increase blood-brain barrier permeability, potentially leading to cerebral vasogenic edema. The cerebrovascular challenges associated with hyperthermia are of paramount importance for populations with compromised thermoregulatory control-for example, spinal cord injury, elderly, and those with preexisting cardiovascular diseases. © 2015 American Physiological Society. Compr Physiol 5:1345-1380, 2015.

AB - This review provides an in-depth update on the impact of heat stress on cerebrovascular functioning. The regulation of cerebral temperature, blood flow, and metabolism are discussed. We further provide an overview of vascular permeability, the neurocognitive changes, and the key clinical implications and pathologies known to confound cerebral functioning during hyperthermia. A reduction in cerebral blood flow (CBF), derived primarily from a respiratory-induced alkalosis, underscores the cerebrovascular changes to hyperthermia. Arterial pressures may also become compromised because of reduced peripheral resistance secondary to skin vasodilatation. Therefore, when hyperthermia is combined with conditions that increase cardiovascular strain, for example, orthostasis or dehydration, the inability to preserve cerebral perfusion pressure further reduces CBF. A reduced cerebral perfusion pressure is in turn the primary mechanism for impaired tolerance to orthostatic challenges. Any reduction in CBF attenuates the brain's convective heat loss, while the hyperthermic-induced increase in metabolic rate increases the cerebral heat gain. This paradoxical uncoupling of CBF to metabolism increases brain temperature, and potentiates a condition whereby cerebral oxygenation may be compromised. With levels of experimentally viable passive hyperthermia (up to 39.5-40.0°C core temperature), the associated reduction in CBF (∼30%) and increase in cerebral metabolic demand (∼10%) is likely compensated by increases in cerebral oxygen extraction. However, severe increases in whole-body and brain temperature may increase blood-brain barrier permeability, potentially leading to cerebral vasogenic edema. The cerebrovascular challenges associated with hyperthermia are of paramount importance for populations with compromised thermoregulatory control-for example, spinal cord injury, elderly, and those with preexisting cardiovascular diseases. © 2015 American Physiological Society. Compr Physiol 5:1345-1380, 2015.

U2 - 10.1002/cphy.c140066

DO - 10.1002/cphy.c140066

M3 - Journal article

C2 - 26140721

VL - 5

SP - 1345

EP - 1380

JO - Comprehensive Physiology

JF - Comprehensive Physiology

SN - 2040-4603

IS - 3

ER -

ID: 142026449