Unknown

Dataset Information

0

Transcription cofactor GRIP1 differentially affects myeloid cell-driven neuroinflammation and response to IFN-? therapy.

ABSTRACT: Macrophages (M?) and microglia (MG) are critical in the pathogenesis of multiple sclerosis (MS) and its mouse model, experimental autoimmune encephalomyelitis (EAE). Glucocorticoids (GCs) and interferon ? (IFN-?) are frontline treatments for MS, and disrupting each pathway in mice aggravates EAE. Glucocorticoid receptor-interacting protein 1 (GRIP1) facilitates both GR and type I IFN transcriptional actions; hence, we evaluated the role of GRIP1 in neuroinflammation. Surprisingly, myeloid cell-specific loss of GRIP1 dramatically reduced EAE severity, immune cell infiltration of the CNS, and MG activation and demyelination specifically during the neuroinflammatory phase of the disease, yet also blunted therapeutic properties of IFN-?. M?/MG transcriptome analyses at the bulk and single-cell levels revealed that GRIP1 deletion attenuated nuclear receptor, inflammatory and, interestingly, type I IFN pathways and promoted the persistence of a homeostatic MG signature. Together, these results uncover the multifaceted function of type I IFN in MS/EAE pathogenesis and therapy, and an unexpectedly permissive role of myeloid cell GRIP1 in neuroinflammation.

SUBMITTER: Mimouna S 

PROVIDER: S-EPMC7555412 | biostudies-literature | 2021 Jan

REPOSITORIES: biostudies-literature

Json Xml
altmetric image

Publications

Transcription cofactor GRIP1 differentially affects myeloid cell-driven neuroinflammation and response to IFN-β therapy.

Mimouna Sanda S   Rollins David A DA   Shibu Gayathri G   Tharmalingam Bowranigan B   Deochand Dinesh K DK   Chen Xi X   Oliver David D   Chinenov Yurii Y   Rogatsky Inez I  

The Journal of experimental medicine 20210101 1

Macrophages (MФ) and microglia (MG) are critical in the pathogenesis of multiple sclerosis (MS) and its mouse model, experimental autoimmune encephalomyelitis (EAE). Glucocorticoids (GCs) and interferon β (IFN-β) are frontline treatments for MS, and disrupting each pathway in mice aggravates EAE. Glucocorticoid receptor-interacting protein 1 (GRIP1) facilitates both GR and type I IFN transcriptional actions; hence, we evaluated the role of GRIP1 in neuroinflammation. Surprisingly, myeloid cell-s  ...[more]

Similar Datasets

Transcriptomics Transcriptionnal coregulator GRIP1 differentially modulate myeloid cell-driven neuroinflammation and response to IFN-beta therapy
2020-10-03 | GSE141721 | GEO
Genomics Transcriptionnal coregulator GRIP1 differentially modulate myeloid cell-driven neuroinflammation and response to IFN-beta therapy
| PRJNA594526 | ENA
Unknown Zika virus infection differentially affects genome-wide transcription in neuronal cells and myeloid dendritic cells.
| S-EPMC7156053 | biostudies-literature
Unknown Hematopoiesis and RAS-driven myeloid leukemia differentially require PI3K isoform p110α.
| S-EPMC3973083 | biostudies-literature
Unknown Glucocorticoid-induced phosphorylation by CDK9 modulates the coactivator functions of transcriptional cofactor GRIP1 in macrophages.
| S-EPMC5700924 | biostudies-literature
Unknown Implications of metabolism-driven myeloid dysfunctions in cancer therapy.
| S-EPMC7570408 | biostudies-literature
Unknown Intensive chemotherapy for acute myeloid leukemia differentially affects circulating TC1, TH1, TH17 and TREG cells.
| S-EPMC2912832 | biostudies-other
Unknown Myeloid cell transmigration across the CNS vasculature triggers IL-1?-driven neuroinflammation during autoimmune encephalomyelitis in mice.
| S-EPMC4886360 | biostudies-literature
Genomics Glucocorticoid-induced phosphorylation by CDK9 specifies the coactivator functions of transcriptional cofactor GRIP1 in macrophages
2017-09-29 | GSE99887 | GEO
Unknown Gene therapy with mesenchymal stem cells expressing IFN-ß ameliorates neuroinflammation in experimental models of multiple sclerosis.
| S-EPMC5241389 | biostudies-literature