| Literature DB >> 12480185 |
Takuya Nikaido1, Ken Iseki, Tetsuji Mori, Hiromi Takaki, Sachihiko Yokoya, Seita Hagino, Junko Takeda, Yuxiang Zhang, Mayumi Takeuchi, Shin-ichi Kikuchi, Akio Wanaka.
Abstract
We reported the expression patterns of a novel member of the CREB/ATF family, OASIS, in central nervous system (CNS) lesions and its transcriptional activity. OASIS gene expression was upregulated in the stab-injured spinal cord. Double labeling experiments revealed that the distribution of OASIS mRNA-positive cells overlapped with a population of GFAP-immunoreactive cells. This finding suggested that OASIS might regulate expression of important downstream molecules in certain subset of the reactive astrocytes (e.g. inhibitory substances in injured brain). In gel shift assays, OASIS was able to specifically bind to CRE as CREB family members were. We then examined transcriptional activity of full-length OASIS with GAL4-UAS-luciferase reporter assay in COS7 cells. OASIS protein activated transcription, but did not inhibit basal transcription driven by AdML promoter. To determine critical portion(s) of the OASIS protein in transcriptional activation, we examined the activity of various deletion constructs of OASIS gene. The assay revealed that a strong transcriptional activation domain lay in the N-terminal region where acidic amino acids clustered and a possible repression domain, which had not been reported for other CREB/ATF family members, lay in the more C-terminal region. We therefore proposed that OASIS protein positively regulated gene transcription in a subset of reactive astrocytes, and thereby influenced the reaction of injured CNS tissues.Entities:
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Year: 2002 PMID: 12480185 DOI: 10.1016/s0169-328x(02)00521-1
Source DB: PubMed Journal: Brain Res Mol Brain Res ISSN: 0169-328X