The Cystine/Glutamate Antiporter, System xc–, Contributes to Cortical Infarction After Moderate but Not Severe Focal Cerebral Ischemia in Mice
Understanding the mechanisms underlying ischemic brain injury is of importance to the goal of devising novel therapeutics for protection and/or recovery. Previous work in our laboratory and in others has shown that activation of cystine/glutamate antiporter, system x c – (Sx c – ), facilitates neuro...
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Published in: | Frontiers in cellular neuroscience Vol. 16; p. 821036 |
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Main Authors: | , |
Format: | Journal Article |
Language: | English |
Published: |
Lausanne
Frontiers Research Foundation
09-05-2022
Frontiers Media S.A |
Subjects: | |
Online Access: | Get full text |
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Summary: | Understanding the mechanisms underlying ischemic brain injury is of importance to the goal of devising novel therapeutics for protection and/or recovery. Previous work in our laboratory and in others has shown that activation of cystine/glutamate antiporter, system x
c
–
(Sx
c
–
), facilitates neuronal injury in several
in vitro
models of energy deprivation. However, studies on the contribution of this antiporter to ischemic brain damage
in vivo
are more limited. Since embolic or thrombotic transient or permanent occlusion of a cerebral blood vessel eventually leads to brain infarction in most stroke cases, we evaluated the contribution of Sx
c
–
to cerebral ischemic damage by comparing brain infarction between mice naturally null for SLC7a11 (SLC7a11
sut/sut
mice) – the gene the encodes for the substrate specific light chain for system x
c
–
– with their wild type (SLC7a11
+ / +
) littermates following photothrombotic ischemic stroke of the middle cerebral artery (PTI) and permanent middle cerebral artery occlusion (pMCAo) rendered by cauterization. In the PTI model, we found a time-dependent reduction in cerebral blood flow that reached 50% from baseline in both genotypes 47–48 h post-illumination. Despite this, a remarkable reduction in incidence and total infarct volume of SLC7a11
sut/sut
mice was revealed 48 h following PTI as compared to SLC7a11
+/+
mice. No difference in injury markers and/or infarct volume was measured between genotypes when occlusion of the MCA was permanent, however. Present data demonstrate a model-dependent differential role for Sx
c
–
in focal cerebral ischemic damage, further highlighting that ischemic severity activates heterogeneous biochemical events that lead to damage engendered by stroke. |
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Bibliography: | ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23 Present address: Yan He, Research and Development Department, Akoya Biosciences, Marlborough, MA, United States Reviewed by: Nikolaus Plesnila, LMU Munich University Hospital, Germany; Jan Lewerenz, University of Ulm, Germany Edited by: Lisa Mapelli, University of Pavia, Italy This article was submitted to Cellular Neurophysiology, a section of the journal Frontiers in Cellular Neuroscience |
ISSN: | 1662-5102 1662-5102 |
DOI: | 10.3389/fncel.2022.821036 |