CCR7 on CD4+ T Cells Plays a Crucial Role in the Induction of Experimental Autoimmune Encephalomyelitis

Belikan, Patrick; Bühler, Ulrike; Wolf, Christina; Pramanik, Gautam; Gollan, René; Zipp, Frauke; Siffrin, Volker

doi:10.4049/jimmunol.1701419

Cited by 27 publications

(14 citation statements)

References 58 publications

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“…5 A, upper panel; GRIP1 deletion efficiency is shown on the right as normalized read counts across "floxed" exon 11 of the Ncoa2 gene). In contrast, more heterogeneous activated CD45 + Cd11b + cells during EAE ( (Belikan et al, 2018;Salter and Stevens, 2017;Scheu et al, 2017). Interestingly, a pool of genes downregulated in WT mice during EAE but persisting in GRIP1-cKO mice (e.g., Gpr34, P2ry12; Fig.…”

Section: Grip1 Regulates the Inflammatory Transcriptome In P0 Mg In Vmentioning

confidence: 94%

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

Mimouna

Rollins

Shibu

et al. 2020

Journal of Experimental Medicine

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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–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-β. MФ/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.

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Section: Grip1 Regulates the Inflammatory Transcriptome In P0 Mg In Vmentioning

confidence: 94%

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

Mimouna

Rollins

Shibu

et al. 2020

Journal of Experimental Medicine

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“…For example, Ccr7 is known to participate in T cell-homeostasis and trafficking 42 and Ccr7 activation by its agonist Ccl21 directly amplifies antigen-specific T cell responses and T cell homeostatic proliferation 43 . Such functions would be relevant to autoimmunity, as Ccr7 promotes Th17-mediated autoimmune disease in experimental dry eye disease 44 , multiple sclerosis (EAE) 45 , and arthritis 46 . Thus, Nod2 may function similar to a co-stimulatory factor to temper the TCR-signaling threshold in order to control antigen-experienced T cells that are self-reactive pathogenic Th17 cells.…”

Section: Discussionmentioning

confidence: 99%

T cell-intrinsic role for Nod2 in protection against Th17-mediated uveitis

et al. 2020

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Mutations in nucleotide-binding oligomerization domain-containing protein 2 (NOD2) cause Blau syndrome, an inflammatory disorder characterized by uveitis. The antimicrobial functions of Nod2 are well-established, yet the cellular mechanisms by which dysregulated Nod2 causes uveitis remain unknown. Here, we report a non-conventional, T cell-intrinsic function for Nod2 in suppression of Th17 immunity and experimental uveitis. Reconstitution of lymphopenic hosts with Nod2−/− CD4+ T cells or retina-specific autoreactive CD4+ T cells lacking Nod2 reveals a T cell-autonomous, Rip2-independent mechanism for Nod2 in uveitis. In naive animals, Nod2 operates downstream of TCR ligation to suppress activation of memory CD4+ T cells that associate with an autoreactive-like profile involving IL-17 and Ccr7. Interestingly, CD4+ T cells from two Blau syndrome patients show elevated IL-17 and increased CCR7. Our data define Nod2 as a T cell-intrinsic rheostat of Th17 immunity, and open new avenues for T cell-based therapies for Nod2-associated disorders such as Blau syndrome.

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“…Specifically, Annexin A6 (ANXA6) has been described to be essential to CD4+ T cell proliferation via interleukin-2 signalling 65 . CCR7, on the other hand, has been predominantly implicated in T cell migration 66 and its deregulation in CD4+ T cells has been associated to several autoimmune diseases including SSc [67][68][69] . Finally, JUND encodes a TF that forms part of the AP-1 complex and has been previously described to regulate T cell proliferation and differentiation 70 .…”

Section: Discussionmentioning

confidence: 99%

Epigenomics and Transcriptomics of Systemic Sclerosis CD4+ T cells reveal Long Range Dysregulation of Key Inflammatory Pathways mediated by disease-associated Susceptibility Loci

Ortíz

Andrés-León

et al. 2020

Preprint

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System sclerosis (SSc) is a genetically complex autoimmune disease mediated by the interplay between genetic and epigenetic factors in a multitude of immune cells, with CD4+ T lymphocytes as one of the principle drivers of pathogenesis. In this study, we obtained DNA methylation and expression profiles of CD4+ T cells from 48 SSc patients and 16 healthy controls. Consequently, we identified 9112 and 3929 differentially methylated CpGs positions (DMPs) and differentially expressed genes (DEGs) respectively. These DMPs and DEGs are enriched in functional categories related to inflammation and T cell biology. Furthermore, correlation analysis identified 17,500 possible DMP-DEG interaction pairs within a window of 5 Mb, and utilizing promoter capture Hi-C data, we confirmed that 212 CD4+ T cel specific pairs of DMP-DEG physically interact involving CTCF. Finally, utilizing SSc GWAS data, we identified four important SSc-associated susceptibility loci, TNIP1 (rs3792783), GSDMB (rs9303277), IL12RB1 (rs2305743) and CSK (rs1378942) , that physically interact with DMP-DEG pairs cg17239269-ANXA6, cg19458020-CCR7, cg10808810-JUND and cg11062629-ULK3 respectively. Overall, our study reveals a solid link between genetic, epigenetic and transcriptional deregulation in CD4+ T cells of SSc patients, providing a novel integrated view of SSc pathogenic determinants.

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CCR7 on CD4+ T Cells Plays a Crucial Role in the Induction of Experimental Autoimmune Encephalomyelitis

Cited by 27 publications

References 58 publications

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

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

T cell-intrinsic role for Nod2 in protection against Th17-mediated uveitis

Epigenomics and Transcriptomics of Systemic Sclerosis CD4+ T cells reveal Long Range Dysregulation of Key Inflammatory Pathways mediated by disease-associated Susceptibility Loci

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