<i>Cnp</i>Promoter-Driven Sustained ERK1/2 Activation Increases B-Cell Activation and Suppresses Experimental Autoimmune Encephalomyelitis

Jeffries, Marisa A.; Obr, Alison E.; Urbanek, Kelly; Fyffe-Maricich, Sharyl L.; Wood, Teresa L.

doi:10.1177/1759091420971916

Cited by 8 publications

(5 citation statements)

References 85 publications

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“…Interestingly, OL cultures lacking PAK1 expression (Figure 7a) had larger myelin membrane surface area than control OLs (Figure 7b,c), while maintaining the same percentage of differentiated OLs relative to the total oligodendroglial population (Figure S5). These results not only confirm that myelin membrane expansion in vitro recapitulates myelin thickening in vivo, but also that myelin thickening in Pak1cKO mice is unlikely to be due to Cnp-Cre recombination in other cell types (Jeffries et al, 2020;Tognatta et al, 2017).…”

Section: Pak1 Deletion In Ols Induces An Increase Of Myelin Thickness...supporting

confidence: 72%

Antagonistic actions of PAK1 and NF2/Merlin drive myelin membrane expansion in oligodendrocytes

Baudouin,

Adès,

Kanté

et al. 2024

Glia

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In the central nervous system, the formation of myelin by oligodendrocytes (OLs) relies on the switch from the polymerization of the actin cytoskeleton to its depolymerization. The molecular mechanisms that trigger this switch have yet to be elucidated. Here, we identified P21‐activated kinase 1 (PAK1) as a major regulator of actin depolymerization in OLs. Our results demonstrate that PAK1 accumulates in OLs in a kinase‐inhibited form, triggering actin disassembly and, consequently, myelin membrane expansion. Remarkably, proteomic analysis of PAK1 binding partners enabled the identification of NF2/Merlin as its endogenous inhibitor. Our findings indicate that Nf2 knockdown in OLs results in PAK1 activation, actin polymerization, and a reduction in OL myelin membrane expansion. This effect is rescued by treatment with a PAK1 inhibitor. We also provide evidence that the specific Pak1 loss‐of‐function in oligodendroglia stimulates the thickening of myelin sheaths in vivo. Overall, our data indicate that the antagonistic actions of PAK1 and NF2/Merlin on the actin cytoskeleton of the OLs are critical for proper myelin formation. These findings have broad mechanistic and therapeutic implications in demyelinating diseases and neurodevelopmental disorders.

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Section: Pak1 Deletion In Ols Induces An Increase Of Myelin Thickness...supporting

confidence: 72%

Antagonistic actions of PAK1 and NF2/Merlin drive myelin membrane expansion in oligodendrocytes

Baudouin,

Adès,

Kanté

et al. 2024

Glia

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“…STAT3 phosphorylation is increased in CD40-activated transitional B cells of healthy subjects but not in those from SLE patients ( 26 ). In addition, CREB, p38 MAPK, ERK1/2, and PI3Kδ have been described to be required for IL-10 upregulation following TLR and/or CD40L stimulation ( 58 , 67 , 110 ). c-Maf, a well-known transactivator of IL-10 in various cell types, has also been shown to mediate IL-10 transcription by LPS-stimulated murine B cells ( 111 ).…”

Section: Regulation Of Il-10 Expression By B Cellsmentioning

confidence: 99%

Immunosuppressive Mechanisms of Regulatory B Cells

et al. 2021

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Regulatory B cells (Bregs) is a term that encompasses all B cells that act to suppress immune responses. Bregs contribute to the maintenance of tolerance, limiting ongoing immune responses and reestablishing immune homeostasis. The important role of Bregs in restraining the pathology associated with exacerbated inflammatory responses in autoimmunity and graft rejection has been consistently demonstrated, while more recent studies have suggested a role for this population in other immune-related conditions, such as infections, allergy, cancer, and chronic metabolic diseases. Initial studies identified IL-10 as the hallmark of Breg function; nevertheless, the past decade has seen the discovery of other molecules utilized by human and murine B cells to regulate immune responses. This new arsenal includes other anti-inflammatory cytokines such IL-35 and TGF-β, as well as cell surface proteins like CD1d and PD-L1. In this review, we examine the main suppressive mechanisms employed by these novel Breg populations. We also discuss recent evidence that helps to unravel previously unknown aspects of the phenotype, development, activation, and function of IL-10-producing Bregs, incorporating an overview on those questions that remain obscure.

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“…In this study, we used tamoxifen-inducible Ng2-Cre ERT ; Mtor fl/fl mice to delete Mtor from adult OPCs that generate new OLs responsible for remyelination. While existing mature OLs appear to contribute to remyelination in the rodent CNS under specific circumstances, such as a motor learning paradigm or genetic modulation (Mason et al, 2000;Bacmeister et al, 2020;Jeffries et al, 2020), published studies indicate that remyelination is otherwise largely a result of new OL production (Targett et al, 1996;Crawford et al, 2016). We show that Mtor deletion from adult OPCs significantly delays remyelination after CPZ demyelination but has no effect on remyelination after LPC demyelination of either the spinal cord or brain, suggesting that Mtor deletion and CPZ treatment may target a similar pathway to impair remyelination.…”

Section: Introductionmentioning

confidence: 99%

mTOR Signaling Regulates Metabolic Function in Oligodendrocyte Precursor Cells and Promotes Efficient Brain Remyelination in the Cuprizone Model

et al. 2021

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In demyelinating diseases, such as multiple sclerosis, primary loss of myelin and subsequent neuronal degeneration throughout the CNS impair patient functionality. While the importance of mechanistic target of rapamycin (mTOR) signaling during developmental myelination is known, no studies have yet directly examined the function of mTOR signaling specifically in the oligodendrocyte (OL) lineage during remyelination. Here, we conditionally deleted Mtor from adult oligodendrocyte precursor cells (OPCs) using Ng2-Cre ERT in male adult mice to test its function in new OLs responsible for remyelination. During early remyelination after cuprizone-induced demyelination, mice lacking mTOR in adult OPCs had unchanged OL numbers but thinner myelin. Myelin thickness recovered by late-stage repair, suggesting a delay in myelin production when Mtor is deleted from adult OPCs. Surprisingly, loss of mTOR in OPCs had no effect on efficiency of remyelination after lysophosphatidylcholine lesions in either the spinal cord or corpus callosum, suggesting that mTOR signaling functions specifically in a pathway dysregulated by cuprizone to promote remyelination efficiency. We further determined that cuprizone and inhibition of mTOR cooperatively compromise metabolic function in primary rat OLs undergoing differentiation. Together, our results support the conclusion that mTOR signaling in OPCs is required to overcome the metabolic dysfunction in the cuprizone-demyelinated adult brain.

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CnpPromoter-Driven Sustained ERK1/2 Activation Increases B-Cell Activation and Suppresses Experimental Autoimmune Encephalomyelitis

Cited by 8 publications

References 85 publications

Antagonistic actions of PAK1 and NF2/Merlin drive myelin membrane expansion in oligodendrocytes

Antagonistic actions of PAK1 and NF2/Merlin drive myelin membrane expansion in oligodendrocytes

Immunosuppressive Mechanisms of Regulatory B Cells

mTOR Signaling Regulates Metabolic Function in Oligodendrocyte Precursor Cells and Promotes Efficient Brain Remyelination in the Cuprizone Model

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