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Publication : Astrocytic transforming growth factor-beta signaling reduces subacute neuroinflammation after stroke in mice.

First Author  Cekanaviciute E Year  2014
Journal  Glia Volume  62
Issue  8 Pages  1227-40
PubMed ID  24733756 Mgi Jnum  J:211178
Mgi Id  MGI:5574231 Doi  10.1002/glia.22675
Citation  Cekanaviciute E, et al. (2014) Astrocytic transforming growth factor-beta signaling reduces subacute neuroinflammation after stroke in mice. Glia 62(8):1227-40
abstractText  Astrocytes limit inflammation after CNS injury, at least partially by physically containing it within an astrocytic scar at the injury border. We report here that astrocytic transforming growth factor-beta (TGFbeta) signaling is a second, distinct mechanism that astrocytes utilize to limit neuroinflammation. TGFbetas are anti-inflammatory and neuroprotective cytokines that are upregulated subacutely after stroke, during a clinically accessible time window. We have previously demonstrated that TGFbetas signal to astrocytes, neurons and microglia in the stroke border days after stroke. To investigate whether TGFbeta affects astrocyte immunoregulatory functions, we engineered "Ast-Tbr2DN" mice where TGFbeta signaling is inhibited specifically in astrocytes. Despite having a similar infarct size to wildtype controls, Ast-Tbr2DN mice exhibited significantly more neuroinflammation during the subacute period after distal middle cerebral occlusion (dMCAO) stroke. The peri-infarct cortex of Ast-Tbr2DN mice contained over 60% more activated CD11b(+) monocytic cells and twice as much immunostaining for the activated microglia and macrophage marker CD68 than controls. Astrocytic scarring was not altered in Ast-Tbr2DN mice. However, Ast-Tbr2DN mice were unable to upregulate TGF-beta1 and its activator thrombospondin-1 2 days after dMCAO. As a result, the normal upregulation of peri-infarct TGFbeta signaling was blunted in Ast-Tbr2DN mice. In this setting of lower TGFbeta signaling and excessive neuroinflammation, we observed worse motor outcomes and late infarct expansion after photothrombotic motor cortex stroke. Taken together, these data demonstrate that TGFbeta signaling is a molecular mechanism by which astrocytes limit neuroinflammation, activate TGFbeta in the peri-infarct cortex and preserve brain function during the subacute period after stroke. GLIA 2014;62:1227-1240.
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