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Park, Sung Ho
Laboratory of Molecular Immunology
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dc.citation.startPage 102347 -
dc.citation.title REDOX BIOLOGY -
dc.citation.volume 54 -
dc.contributor.author Kim, Sinai -
dc.contributor.author Lee, Wonhyo -
dc.contributor.author Jo, Huiju -
dc.contributor.author Sonn, Seong-Keun -
dc.contributor.author Jeong, Se-Jin -
dc.contributor.author Seo, Seungwoon -
dc.contributor.author Suh, Joowon -
dc.contributor.author Jin, Jing -
dc.contributor.author Kweon, Hyae Yon -
dc.contributor.author Kim, Tae Kyeong -
dc.contributor.author Moon, Shin Hye -
dc.contributor.author Jeon, Sejin -
dc.contributor.author Kim, Jong Woo -
dc.contributor.author Kim, Yu Ri -
dc.contributor.author Lee, Eun-Woo -
dc.contributor.author Shin, Hwa Kyoung -
dc.contributor.author Park, Sung Ho -
dc.contributor.author Oh, Goo Taeg -
dc.date.accessioned 2023-12-21T13:43:56Z -
dc.date.available 2023-12-21T13:43:56Z -
dc.date.created 2023-01-02 -
dc.date.issued 2022-08 -
dc.description.abstract Ischemic stroke is the leading cause of immortal disability and death worldwide. For treatment in the acute phase, it is necessary to control excessive reactive oxygen species (ROS) damage during ischemia/reperfusion (I/ R). Microglia are well known to be closely associated with excessive ROS response in the early stage of I/R. However, the precise roles of microglia associated with mitigating ROS damage, and molecular markers of heterogenetic microglia in the I/R damaged brain has not been clarified. Here, we identified a new type of microglia associated with stroke in the I/R injured brain. Single-cell RNA sequencing (scRNA-seq) was used to assess transcriptional changes of microglia and immune cells in the contralateral (CL) and ipsilateral (IL) hemispheres after transient middle cerebral artery occlusion (tMCAO) surgery to mimic ischemic stroke. We classified a unique type of microglia with enhanced antioxidant function and markers similar to those of disease associated microglia (DAM), designated them as stroke-associated microglia (SAM). The representative antioxidant enzyme, Peroxiredoxin-1 (Prdx1), was predominantly expressed in SAM and mediated ROS defense genes, including Txn1, Srx1, Mt1, and Mt2. In the Prdx1(-/-) I/R damaged brain, we observed significantly increased infarction, as assessed by TTC staining, and FACS analysis detected severe microglial cell death. Importantly, scRNA transcriptomics data showed that the SAM population was specifically decreased in Prdx1-/- mice and that these mice exhibited decreased ROS damage resistance. Inflammatory responses which were detected by ELISA and qPCR, were also increased in Prdx1-/- IL hemispheres. Finally, Prdx1-dependent antioxidative SAM were found to be essential for increasing the transcription levels of stroke-protective molecules, such as osteopontin and ferritin. A novel microglia type (SAM) is specifically activated in response to stroke I/R injury, and that Prdx1 expression is required for the activation and enhanced antioxidant function of SAM. -
dc.identifier.bibliographicCitation REDOX BIOLOGY, v.54, pp.102347 -
dc.identifier.doi 10.1016/j.redox.2022.102347 -
dc.identifier.issn 2213-2317 -
dc.identifier.scopusid 2-s2.0-85131680181 -
dc.identifier.uri https://scholarworks.unist.ac.kr/handle/201301/60723 -
dc.identifier.url https://www.sciencedirect.com/science/article/pii/S2213231722001197?via%3Dihub -
dc.identifier.wosid 000811997200001 -
dc.language 영어 -
dc.publisher ELSEVIER -
dc.title The antioxidant enzyme Peroxiredoxin-1 controls stroke-associated microglia against acute ischemic stroke -
dc.type Article -
dc.description.isOpenAccess FALSE -
dc.relation.journalWebOfScienceCategory Biochemistry & Molecular Biology -
dc.relation.journalResearchArea Biochemistry & Molecular Biology -
dc.type.docType Article -
dc.description.journalRegisteredClass scie -
dc.description.journalRegisteredClass scopus -
dc.subject.keywordAuthor Ischemic stroke -
dc.subject.keywordAuthor Stroke-associated microglia (SAM) -
dc.subject.keywordAuthor Reactive oxygen species (ROS) -
dc.subject.keywordAuthor Peroxiredoxin-1 (Prdx1) -
dc.subject.keywordAuthor Single cell RNA sequencing -
dc.subject.keywordPlus CENTRAL-NERVOUS-SYSTEM -
dc.subject.keywordPlus IMMUNE CELLS -
dc.subject.keywordPlus BRAIN -
dc.subject.keywordPlus INFLAMMATION -
dc.subject.keywordPlus ACCUMULATION -
dc.subject.keywordPlus OSTEOPONTIN -
dc.subject.keywordPlus MACROPHAGE -
dc.subject.keywordPlus CLEARANCE -
dc.subject.keywordPlus DEFICIENT -
dc.subject.keywordPlus DYNAMICS -

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