Influence of sex, age and diabetes on brain transcriptome and proteome modifications following cerebral ischemia

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作者
Laura Ramiro
Júlia Faura
Alba Simats
Paula García-Rodríguez
Feifei Ma
Luna Martín
Francesc Canals
Anna Rosell
Joan Montaner
机构
[1] Vall d’Hebron Institute of Research (VHIR),Neurovascular Research Laboratory
[2] Universitat Autònoma de Barcelona,Proteomics Laboratory, Vall d’Hebron Institute of Oncology (VHIO)
[3] Universitat Autònoma de Barcelona, Stroke Research Program, Institute of Biomedicine of Seville, IBiS/Hospital Universitario Virgen del Rocío/CSIC/University of Seville & Department of Neurology
[4] Hospital Universitario Virgen Macarena,undefined
来源
BMC Neuroscience | / 24卷
关键词
Ischemic stroke; Proteome; Transcriptome; Sex; Diabetes; Age;
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摘要
Ischemic stroke is a major cause of death and disability worldwide. Translation into the clinical setting of neuroprotective agents showing promising results in pre-clinical studies has systematically failed. One possible explanation is that the animal models used to test neuroprotectants do not properly represent the population affected by stroke, as most of the pre-clinical studies are performed in healthy young male mice. Therefore, we aimed to determine if the response to cerebral ischemia differed depending on age, sex and the presence of comorbidities. Thus, we explored proteomic and transcriptomic changes triggered during the hyperacute phase of cerebral ischemia (by transient intraluminal middle cerebral artery occlusion) in the brain of: (1) young male mice, (2) young female mice, (3) aged male mice and (4) diabetic young male mice. Moreover, we compared each group's proteomic and transcriptomic changes using an integrative enrichment pathways analysis to disclose key common and exclusive altered proteins, genes and pathways in the first stages of the disease. We found 61 differentially expressed genes (DEG) in male mice, 77 in females, 699 in diabetics and 24 in aged mice. Of these, only 14 were commonly dysregulated in all groups. The enrichment pathways analysis revealed that the inflammatory response was the biological process with more DEG in all groups, followed by hemopoiesis. Our findings indicate that the response to cerebral ischemia regarding proteomic and transcriptomic changes differs depending on sex, age and comorbidities, highlighting the importance of incorporating animals with different phenotypes in future stroke research studies.
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