Contributors: Department of Clinical Sciences; Laboratory for Experimental Brain Research; Skane University Hospital Lund -Skane University Hospital Lund; Neuroinflammation Unit; Biotech Research and Innovation Centre-University of Copenhagen = Københavns Universitet (UCPH); Department of Neurobiology Research; University of Southern Denmark (SDU)-Institute of Molecular Medicine; Department of Experimental Medical Sciences Lund; Skane University Hospital Lund; This work was supported by grants from: Fundação para a Ciência e aTecnologia (ARI), Portugal; A.E. Berger, The Crafoord Foundation, G.E. Kock’sFoundation, The Gyllenstiernska Krapperup Foundation, The Royal PhysiographicSociety in Lund, Swedish National Stroke Foundation, and the Swedish ResearchCouncil grant no. 2012–2229 (TD), Sweden; The Danish Independent ResearchCouncil, and The Lundbeck Foundation (SI-N), Denmark; Brødrene HartmannFond (BHC), Savværksejer Jeppe Juhl og Hustru Ovita Juhls Mindelegat (KLL),and The Lundbeck Foundation (BHC and KLL), Denmark; Agency for Researchand Innovation, Council for Health Research (RK supported by a grant to TrevorOwens), Denmark
نبذة مختصرة : International audience ; AbstractBackgroundInterferon (IFN)-β exerts anti-inflammatory effects, coupled to remarkable neurological improvements in multiple sclerosis, a neuroinflammatory condition of the central nervous system. Analogously, it has been hypothesized that IFN-β, by limiting inflammation, decreases neuronal death and promotes functional recovery after stroke. However, the core actions of endogenous IFN-β signaling in stroke are unclear.MethodsTo address this question, we used two clinically relevant models of focal cerebral ischemia, transient and permanent middle cerebral artery occlusion, and two genetically modified mouse lines, lacking either IFN-β or its receptor, the IFN-α/β receptor. Subsets of inflammatory and immune cells isolated from the brain, blood, and spleen were studied using flow cytometry. Sensorimotor deficits were assessed by a modified composite neuroscore, the rotating pole and grip strength tests, and cerebral infarct volumes were given by lack of neuronal nuclei immunoreactivity.ResultsHere, we report alterations in local and systemic inflammation in IFN-β knockout (IFN-βKO) mice over 8 days after induction of focal cerebral ischemia. Notably, IFN-βKO mice showed a higher number of infiltrating leukocytes in the brain 2 days after stroke. Concomitantly, in the blood of IFN-βKO mice, we found a higher percentage of total B cells but a similar percentage of mature and activated B cells, collectively indicating a higher proliferation rate. The additional differential regulation of circulating cytokines and splenic immune cell populations in wild-type and IFN-βKO mice further supports an important immunoregulatory function of IFN-β in stroke. Moreover, we observed a significant weight loss 2–3 days and a reduction in grip strength 2 days after stroke in the IFN-βKO group, while endogenous IFN-β signaling did not affect the infarct volume.ConclusionsWe conclude that endogenous IFN-β signaling attenuates local inflammation, regulates peripheral immune cells, and, thereby, may ...
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