Breakdown in repression of IFN-y mRNA leads to accumulation of self-reactive effector CD8+ T Cells
Description
Free to read
Tight regulation of virus-induced cytotoxic effector CD8+ T cells is essential to prevent immunopathology. Naturally occurring effector CD8+ T cells, with a KLRG1hi CD62Llo phenotype typical of short-lived effector CD8+ T cells (SLECs), can be found in increased numbers in autoimmune-prone mice, most notably in mice homozygous for the san allele of Roquin. These SLEC-like cells were able to trigger autoimmune diabetes in a susceptible background. When Roquin is mutated (Roquinsan), effector CD8+ T cells accumulate in a cell-autonomous manner, most prominently as SLEC-like effectors. Excessive IFN-γ promotes the accumulation of SLEC-like cells, increases their T-bet expression, and enhances their granzyme B production in vivo. We show that overexpression of IFN-γ was caused by failed posttranscriptional repression of Ifng mRNA. This study identifies a novel mechanism that prevents accumulation of self-reactive cytotoxic effectors, highlighting the importance of regulating Ifng mRNA stability to maintain CD8+ T cell homeostasis and prevent CD8-mediated autoimmunity.
Impact and interest:
Citation counts are sourced monthly from Scopus and Web of Science® citation databases.
These databases contain citations from different subsets of available publications and different time periods and thus the citation count from each is usually different. Some works are not in either database and no count is displayed. Scopus includes citations from articles published in 1996 onwards, and Web of Science® generally from 1980 onwards.
Citations counts from the Google Scholar™ indexing service can be viewed at the linked Google Scholar™ search.
| ID Code: | 106830 | ||
|---|---|---|---|
| Item Type: | Contribution to Journal (Journal Article) | ||
| Refereed: | Yes | ||
| ORCID iD: |
|
||
| Measurements or Duration: | 10 pages | ||
| Keywords: | *Cytotoxicity, Adoptive Transfer, Animals, C-Type/biosynthesis/genetics, CD8-Positive T-Lymphocytes/*immunology/pathology/transplantation, Cell Aggregation/genetics/*immunology, Cell Aging/genetics/immunology, Down-Regulation/genetics/*immunology, Homeostasis/genetics/immunology, Immunologic/genetics, Immunosuppressive Agents/antagonists & inhibitors/metabolism, Inbred C57BL, Interferon-gamma/*antagonists & inhibitors/biosynthesis/*genetics, Knockout, Lectins, Messenger/*antagonists & inhibitors/genetics, Mice, Mutation/immunology, RNA, RNA Stability/immunology, Trans-Activators/biosynthesis/genetics, Transgenic, Ubiquitin-Protein Ligases/genetics | ||
| DOI: | 10.4049/jimmunol.1102432 | ||
| ISSN: | 0022-1767 | ||
| Pure ID: | 32413855 | ||
| Divisions: | Past > QUT Faculties & Divisions > Faculty of Health Past > Institutes > Institute of Health and Biomedical Innovation |
||
| Copyright Owner: | Consult author(s) regarding copyright matters | ||
| Copyright Statement: | This work is covered by copyright. Unless the document is being made available under a Creative Commons Licence, you must assume that re-use is limited to personal use and that permission from the copyright owner must be obtained for all other uses. If the document is available under a Creative Commons License (or other specified license) then refer to the Licence for details of permitted re-use. It is a condition of access that users recognise and abide by the legal requirements associated with these rights. If you believe that this work infringes copyright please provide details by email to qut.copyright@qut.edu.au | ||
| Deposited On: | 12 May 2017 02:04 | ||
| Last Modified: | 01 Mar 2024 13:13 |
Export: EndNote | Dublin Core | BibTeX
Repository Staff Only: item control page
CORE (COnnecting REpositories)
CORE (COnnecting REpositories)