The role of Ets2 transcription factor in the induction of microRNA-155 by LPS, and its targeting by IL-10.
Loading...
Date
Authors
Journal Title
Journal ISSN
Volume Title
Publisher
Access
OpenAccess
Embargo end date
Citation
Quinn SR, Mangan NE, Caffrey BE, Gantier MP, Williams BR, Hertzog PJ, McCoy CE, O'Neill LA., The role of Ets2 transcription factor in the induction of microRNA-155 by LPS, and its targeting by IL-10., The Journel of Biological Chemistry, 289, 9, 2014, 4316-4325
Abstract
MicroRNA-155 (miR-155) is highly
expressed in many cancers such as B cell
lymphomas and myeloid leukaemia, and
inflammatory disorders such as
rheumatoid arthritis, atopic dermatitis
and multiple sclerosis. The role of miR-
155 as both a promoter of inflammation
and an oncogenic agent provides a clear
need for miR-155 itself to be stringently
regulated. We therefore investigated the
transcriptional regulation of miR-155 in
response to the respective pro- and antiinflammatory
mediators LPS and IL-10.
Bioinformatic analysis revealed Ets
binding sites on the miR-155 promoter,
and we found that Ets2 is critical for miR-
155 induction by LPS. Truncation and
mutational analysis of the miR-155
promoter confirmed the role of the Ets2
binding site proximal to the transcription
start site for LPS responsiveness. We
observed increased binding of Ets2 to the
miR-155 promoter and Ets2 deficient
mice displayed decreased induction of
miR-155 in response to LPS. IL-10
inhibited the induction of Ets2 mRNA
and protein by LPS, thereby decreasing
Ets2 function on the pri-155 promoter.
We have thus identified Ets2 as a key
novel regulator in both the positive and
negative control of miR-155 in the
inflammatory response.
Description
PUBLISHED
Endorsement
Review
Supplemented By
Referenced By
Keywords
Sponsor: Australian Research Council (ARC)
Sponsor: Science Foundation Ireland (SFI)
Sponsor: European Research Council (ERC)
Sponsor: Health Research Board (HRB)
Author's Homepage: http://people.tcd.ie/laoneill
Type of material: Journal Article

