Alcohol exposure–induced neurovascular inflammatory priming impacts ischemic stroke and is linked with brain perivascular macrophages
Antoine Drieu, Anastasia Lanquetin, Damien Levard, Martina Glavan, Francisco Campos, Aurélien Quenault, Eloïse Lemarchand, Mikaël Naveau, Anne Lise Pitel, José Castillo, Denis Vivien, Marina Rubio
Antoine Drieu, Anastasia Lanquetin, Damien Levard, Martina Glavan, Francisco Campos, Aurélien Quenault, Eloïse Lemarchand, Mikaël Naveau, Anne Lise Pitel, José Castillo, Denis Vivien, Marina Rubio
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Research Article Inflammation Neuroscience

Alcohol exposure–induced neurovascular inflammatory priming impacts ischemic stroke and is linked with brain perivascular macrophages

Abstract

Alcohol abuse is a major public health problem worldwide, causing a wide range of preventable morbidity and mortality. In this translational study, we show that heavy drinking (HD) (≥6 standard drinks/day) is independently associated with a worse outcome for ischemic stroke patients. To study the underlying mechanisms of this deleterious effect of HD, we performed an extensive analysis of the brain inflammatory responses of mice chronically exposed or not to 10% alcohol before and after ischemic stroke. Inflammatory responses were analyzed at the parenchymal, perivascular, and vascular levels by using transcriptomic, immunohistochemical, in vivo 2-photon microscopy and molecular MRI analyses. Alcohol-exposed mice show, in the absence of any other insult, a neurovascular inflammatory priming (i.e., an abnormal inflammatory status including an increase in brain perivascular macrophages [PVM]) associated with exacerbated inflammatory responses after a secondary insult (ischemic stroke or LPS challenge). Similar to our clinical data, alcohol-exposed mice showed larger ischemic lesions. We show here that PVM are key players on this aggravating effect of alcohol, since their specific depletion blocks the alcohol-induced aggravation of ischemic lesions. This study opens potentially new therapeutic avenues aiming at blocking alcohol-induced exacerbation of the neurovascular inflammatory responses triggered after ischemic stroke.

Authors

Antoine Drieu, Anastasia Lanquetin, Damien Levard, Martina Glavan, Francisco Campos, Aurélien Quenault, Eloïse Lemarchand, Mikaël Naveau, Anne Lise Pitel, José Castillo, Denis Vivien, Marina Rubio

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Figure 6

Alcohol exposure increases vascular inflammatory responses after ischemic stroke in mice.

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Alcohol exposure increases vascular inflammatory responses after ischemi...
(A) Representative photomicrographs of P-selectin immunostaining in control and alcohol-exposed mice 24 hours after stroke onset. Scale bars: 50 μm. (B) Quantification of the number of P-selectin+ vessels. (C) Quantification of P-selectin+ immunostaining area. (D) Representative T2*-weighted images of in vivo P-selectin molecular imaging. Arrows show MPIO+ blood vessels (n = 5–6 mice/group). (E) Quantification of MPIO+ area. (F) Quantification of MPIO+ blood vessels. (G) Schematic view of the craniotomy performed for thrombin injection, which leads to the occlusion of the MCA and the thinned-skull window for intravital 2-photon imaging. (H) Compilation of representative time-lapse images showing in vivo leukocyte adhesion (arrows) obtained by 2-photon microscopy. Scale bars: 50 μm. (I) Quantification of leukocyte adhesion. (J) Representative time-lapse images of in vivo leukocyte rolling. Scale bars: 50 μm. (K) Quantification of leukocyte rolling (see also Supplemental Videos 3 and 4). n = 4 mice per group. *P < 0.05 versus control, Mann-Whitney U test.