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Age-specific transcriptional response to stroke
Authors:Matthias W. Sieber  Madlen Guenther  Nadine Jaenisch  Daniela Albrecht-Eckardt  Matthias Kohl  Otto W. Witte  Christiane Frahm
Affiliation:1. Hans Berger Department of Neurology, Jena University Hospital, Friedrich Schiller University, Jena, Germany;2. CSCC, Center for Sepsis Control and Care, Jena University Hospital, Jena, Germany;3. Biocontrol Jena GmbH, Jena, Germany;4. Department of Mechanical and Process Engineering, Furtwangen University, Villingen-Schwenningen, Germany
Abstract:
Increased age is a major risk factor for stroke incidence and post-ischemic mortality. To develop age-adjusted therapeutic interventions, a clear understanding of the complexity of age-related post-ischemic mechanisms is essential. Transient occlusion of the middle cerebral artery—a model that closely resembles human stroke—was used to induce cerebral infarction in mice of 4 different ages (2, 9, 15, 24 months). By using Illumina cDNA microarrays and quantitative PCR we detected a distinct age-dependent response to stroke involving 350 differentially expressed genes. Our analyses also identified 327 differentially expressed genes that responded to stroke in an age-independent manner. These genes are involved in different aspects of the inflammatory and immune response, oxidative stress, cell cycle activation and/or DNA repair, apoptosis, cytoskeleton reorganization and/or astrogliosis, synaptic plasticity and/or neurotransmission, and depressive disorders and/or dopamine-, serotonin-, GABA-signaling. In agreement with our earlier work, aged brains displayed an attenuated inflammatory and immune response (Sieber et al., 2011) and a reduced impairment of post-stroke synaptic plasticity. Our data also revealed a distinct age-related susceptibility for post-ischemic depression, the most common neuropsychiatric consequence of stroke, which has a major influence on functional outcome.
Keywords:MCAO   Inflammation   Aging   Depression
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