Author: Hamo, Ludwig; Stohlman, Stephen A.; Ottoâ€Duessel, Maya; Bergmann, Cornelia C.
Title: Distinct regulation of MHC molecule expression on astrocytes and microglia during viral encephalomyelitis Cord-id: t7vav41i Document date: 2007_6_28
ID: t7vav41i
Snippet: The potential interplay of glial cells with T cells during viral induced inflammation was assessed by comparing major histocompatibility complex molecule upregulation and retention on astrocytes and microglia. Transgenic mice expressing green fluorescent protein under control of the astrocyteâ€specific glial fibrillary acidic protein promoter were infected with a neurotropic coronavirus to facilitate phenotypic characterization of astrocytes and microglia using flow cytometry. Astrocytes in the
Document: The potential interplay of glial cells with T cells during viral induced inflammation was assessed by comparing major histocompatibility complex molecule upregulation and retention on astrocytes and microglia. Transgenic mice expressing green fluorescent protein under control of the astrocyteâ€specific glial fibrillary acidic protein promoter were infected with a neurotropic coronavirus to facilitate phenotypic characterization of astrocytes and microglia using flow cytometry. Astrocytes in the adult central nervous system upâ€regulated class I surface expression, albeit delayed compared with microglia. Class II was barely detectable on astrocytes, in contrast to potent upâ€regulation on microglia. Maximal MHC expression in both glial cell types correlated with IFNâ€Î³ levels and lymphocyte accumulation. Despite a decline of IFNâ€Î³ concomitant to virus clearance, MHC molecule expression on glia was sustained. These data demonstrate distinct regulation of both class I and class II expression by microglia and astrocytes in vivo following viral induced inflammation. Furthermore, prolonged MHC expression subsequent to viral clearance implies a potential for ongoing presentation. © 2007 Wileyâ€Liss, Inc.
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