Translatome analysis in acute ischemic stroke: Astrocytes and microglia exhibit differences in poststroke alternative splicing of expressed transcripts

Bingxue Jin(Capital Medical University), Yilai Han(Capital Medical University), Fang Xu(Capital Medical University), Junjie Wang(Capital Medical University), Yunzhi Zhao(Capital Medical University), Haijie Liu(Capital Medical University), Fei Wang(Capital Medical University), Ze Wang(Capital Medical University), Wanting Lu(Capital Medical University), Mingyang Wang(Capital Medical University), Lili Cui(Capital Medical University), Yinan Zhao(Capital Medical University), Junwei Hao(Ministry of Education of the People's Republic of China), Guoliang Chai(Ministry of Education of the People's Republic of China)
The FASEB Journal
August 3, 2024
Cited by 3Open Access
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Abstract

Astrocytes and microglia undergo dynamic and complex morphological and functional changes following ischemic stroke, which are instrumental in both inflammatory responses and neural repair. While gene expression alterations poststroke have been extensively studied, investigations into posttranscriptional regulatory mechanisms, specifically alternative splicing (AS), remain limited. Utilizing previously reported Ribo-Tag-seq data, this study analyzed AS alterations in poststroke astrocytes and microglia from young adult male and female mice. Our findings reveal that in astrocytes, compared to the sham group, 109 differential alternative splicing (DAS) events were observed at 4 h poststroke, which increased to 320 at day 3. In microglia, these numbers were 316 and 266, respectively. Interestingly, the disparity between DAS genes and differentially expressed genes is substantial, with fewer than 10 genes shared at both poststroke time points in astrocytes and microglia. Gene ontology enrichment analysis revealed the involvement of these DAS genes in diverse functions, encompassing immune response (Adam8, Ccr1), metabolism (Acsl6, Pcyt2, Myo5a), and developmental cell growth (App), among others. Selective DAS events were further validated by semiquantitative RT-PCR. Overall, this study comprehensively describes the AS alterations in astrocytes and microglia during the hyperacute and acute phases of ischemic stroke and underscores the significance of certain hub DAS events in neuroinflammatory processes.


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