Anesthesia-Induced Hypothermia Attenuates Early-Phase Blood-Brain Barrier Disruption but Not Infarct Volume following Cerebral Ischemia

Blood-brain barrier (BBB) disruption is thought to facilitate the development of cerebral infarction after a stroke. In a typical stroke model (such as the one used in this study), the early phase of BBB disruption reaches a peak 6 h post-ischemia and largely recovers after 8–24 h, whereas the late...

Descripción completa

Detalles Bibliográficos
Autores principales: Liu, Yu-Cheng, Lee, Yu-Da, Wang, Hwai-Lee, Liao, Kate Hsiurong, Chen, Kuen-Bao, Poon, Kin-Shing, Pan, Yu-Ling, Lai, Ted Weita
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5261567/
https://www.ncbi.nlm.nih.gov/pubmed/28118390
http://dx.doi.org/10.1371/journal.pone.0170682
_version_ 1782499602881052672
author Liu, Yu-Cheng
Lee, Yu-Da
Wang, Hwai-Lee
Liao, Kate Hsiurong
Chen, Kuen-Bao
Poon, Kin-Shing
Pan, Yu-Ling
Lai, Ted Weita
author_facet Liu, Yu-Cheng
Lee, Yu-Da
Wang, Hwai-Lee
Liao, Kate Hsiurong
Chen, Kuen-Bao
Poon, Kin-Shing
Pan, Yu-Ling
Lai, Ted Weita
author_sort Liu, Yu-Cheng
collection PubMed
description Blood-brain barrier (BBB) disruption is thought to facilitate the development of cerebral infarction after a stroke. In a typical stroke model (such as the one used in this study), the early phase of BBB disruption reaches a peak 6 h post-ischemia and largely recovers after 8–24 h, whereas the late phase of BBB disruption begins 48–58 h post-ischemia. Because cerebral infarct develops within 24 h after the onset of ischemia, and several therapeutic agents have been shown to reduce the infarct volume when administered at 6 h post-ischemia, we hypothesized that attenuating BBB disruption at its peak (6 h post-ischemia) can also decrease the infarct volume measured at 24 h. We used a mouse stroke model obtained by combining 120 min of distal middle cerebral arterial occlusion (dMCAo) with ipsilateral common carotid arterial occlusion (CCAo). This model produced the most reliable BBB disruption and cerebral infarction compared to other models characterized by a shorter duration of ischemia or obtained with dMCAO or CCAo alone. The BBB permeability was measured by quantifying Evans blue dye (EBD) extravasation, as this tracer has been shown to be more sensitive for the detection of early-phase BBB disruption compared to other intravascular tracers that are more appropriate for detecting late-phase BBB disruption. We showed that a 1 h-long treatment with isoflurane-anesthesia induced marked hypothermia and attenuated the peak of BBB disruption when administered 6 h after the onset of dMCAo/CCAo-induced ischemia. We also demonstrated that the inhibitory effect of isoflurane was hypothermia-dependent because the same treatment had no effect on ischemic BBB disruption when the mouse body temperature was maintained at 37°C. Importantly, inhibiting the peak of BBB disruption by hypothermia had no effect on the volume of brain infarct 24 h post-ischemia. In conclusion, inhibiting the peak of BBB disruption is not an effective neuroprotective strategy, especially in comparison to the inhibitors of the neuronal death signaling cascade; these, in fact, can attenuate the infarct volume measured at 24 h post-ischemia when administered at 6 h in our same stroke model.
format Online
Article
Text
id pubmed-5261567
institution National Center for Biotechnology Information
language English
publishDate 2017
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-52615672017-02-17 Anesthesia-Induced Hypothermia Attenuates Early-Phase Blood-Brain Barrier Disruption but Not Infarct Volume following Cerebral Ischemia Liu, Yu-Cheng Lee, Yu-Da Wang, Hwai-Lee Liao, Kate Hsiurong Chen, Kuen-Bao Poon, Kin-Shing Pan, Yu-Ling Lai, Ted Weita PLoS One Research Article Blood-brain barrier (BBB) disruption is thought to facilitate the development of cerebral infarction after a stroke. In a typical stroke model (such as the one used in this study), the early phase of BBB disruption reaches a peak 6 h post-ischemia and largely recovers after 8–24 h, whereas the late phase of BBB disruption begins 48–58 h post-ischemia. Because cerebral infarct develops within 24 h after the onset of ischemia, and several therapeutic agents have been shown to reduce the infarct volume when administered at 6 h post-ischemia, we hypothesized that attenuating BBB disruption at its peak (6 h post-ischemia) can also decrease the infarct volume measured at 24 h. We used a mouse stroke model obtained by combining 120 min of distal middle cerebral arterial occlusion (dMCAo) with ipsilateral common carotid arterial occlusion (CCAo). This model produced the most reliable BBB disruption and cerebral infarction compared to other models characterized by a shorter duration of ischemia or obtained with dMCAO or CCAo alone. The BBB permeability was measured by quantifying Evans blue dye (EBD) extravasation, as this tracer has been shown to be more sensitive for the detection of early-phase BBB disruption compared to other intravascular tracers that are more appropriate for detecting late-phase BBB disruption. We showed that a 1 h-long treatment with isoflurane-anesthesia induced marked hypothermia and attenuated the peak of BBB disruption when administered 6 h after the onset of dMCAo/CCAo-induced ischemia. We also demonstrated that the inhibitory effect of isoflurane was hypothermia-dependent because the same treatment had no effect on ischemic BBB disruption when the mouse body temperature was maintained at 37°C. Importantly, inhibiting the peak of BBB disruption by hypothermia had no effect on the volume of brain infarct 24 h post-ischemia. In conclusion, inhibiting the peak of BBB disruption is not an effective neuroprotective strategy, especially in comparison to the inhibitors of the neuronal death signaling cascade; these, in fact, can attenuate the infarct volume measured at 24 h post-ischemia when administered at 6 h in our same stroke model. Public Library of Science 2017-01-24 /pmc/articles/PMC5261567/ /pubmed/28118390 http://dx.doi.org/10.1371/journal.pone.0170682 Text en © 2017 Liu et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Liu, Yu-Cheng
Lee, Yu-Da
Wang, Hwai-Lee
Liao, Kate Hsiurong
Chen, Kuen-Bao
Poon, Kin-Shing
Pan, Yu-Ling
Lai, Ted Weita
Anesthesia-Induced Hypothermia Attenuates Early-Phase Blood-Brain Barrier Disruption but Not Infarct Volume following Cerebral Ischemia
title Anesthesia-Induced Hypothermia Attenuates Early-Phase Blood-Brain Barrier Disruption but Not Infarct Volume following Cerebral Ischemia
title_full Anesthesia-Induced Hypothermia Attenuates Early-Phase Blood-Brain Barrier Disruption but Not Infarct Volume following Cerebral Ischemia
title_fullStr Anesthesia-Induced Hypothermia Attenuates Early-Phase Blood-Brain Barrier Disruption but Not Infarct Volume following Cerebral Ischemia
title_full_unstemmed Anesthesia-Induced Hypothermia Attenuates Early-Phase Blood-Brain Barrier Disruption but Not Infarct Volume following Cerebral Ischemia
title_short Anesthesia-Induced Hypothermia Attenuates Early-Phase Blood-Brain Barrier Disruption but Not Infarct Volume following Cerebral Ischemia
title_sort anesthesia-induced hypothermia attenuates early-phase blood-brain barrier disruption but not infarct volume following cerebral ischemia
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5261567/
https://www.ncbi.nlm.nih.gov/pubmed/28118390
http://dx.doi.org/10.1371/journal.pone.0170682
work_keys_str_mv AT liuyucheng anesthesiainducedhypothermiaattenuatesearlyphasebloodbrainbarrierdisruptionbutnotinfarctvolumefollowingcerebralischemia
AT leeyuda anesthesiainducedhypothermiaattenuatesearlyphasebloodbrainbarrierdisruptionbutnotinfarctvolumefollowingcerebralischemia
AT wanghwailee anesthesiainducedhypothermiaattenuatesearlyphasebloodbrainbarrierdisruptionbutnotinfarctvolumefollowingcerebralischemia
AT liaokatehsiurong anesthesiainducedhypothermiaattenuatesearlyphasebloodbrainbarrierdisruptionbutnotinfarctvolumefollowingcerebralischemia
AT chenkuenbao anesthesiainducedhypothermiaattenuatesearlyphasebloodbrainbarrierdisruptionbutnotinfarctvolumefollowingcerebralischemia
AT poonkinshing anesthesiainducedhypothermiaattenuatesearlyphasebloodbrainbarrierdisruptionbutnotinfarctvolumefollowingcerebralischemia
AT panyuling anesthesiainducedhypothermiaattenuatesearlyphasebloodbrainbarrierdisruptionbutnotinfarctvolumefollowingcerebralischemia
AT laitedweita anesthesiainducedhypothermiaattenuatesearlyphasebloodbrainbarrierdisruptionbutnotinfarctvolumefollowingcerebralischemia

Ejemplares similares