Chromatin-Remodeling Factor Brg1 Is Required for Schwann Cell Differentiation and Myelination

Weider, Matthias; Küspert, Melanie; Bischof, Melanie; Vogl, Michael; Hornig, Julia; Loy, Kristina; Kosian, Thomas; Müller, Jana; Hillgärtner, Simone; Tamm, Ernst R.; Metzger, Daniel

doi:10.1016/j.devcel.2012.05.017

Cited by 106 publications

(139 citation statements)

References 36 publications

(63 reference statements)

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“…Both Brg1 and Baf155 heterozygous mutants exhibit neural tube closure defects and exencephaly, suggesting that BAF complexes have an important and dosage-sensitive role in neural differentiation and development (Bultman et al, 2000;Kim et al, 2001). In agreement with these observations, BRG1 is required during both neuronal and glial differentiation (Marathe et al, 2013;Matsumoto et al, 2006;Weider et al, 2012;Yu et al, 2013). In the central nervous system, the differentiation of glial progenitor cells to form first immature and subsequently mature myelinating oligodendrocytes requires BRG1 (Yu et al, 2013).…”

Section: Baf Complexes In Neural Developmentsupporting

confidence: 67%

“…This combination of transcription factor, chromatin remodeler and activating histone mark drives oligodendrocyte differentiation and myelination. In the peripheral nervous system, BAF complexes are essential for the differentiation of Schwann cells (Weider et al, 2012). Here, SOX10, a Schwann cell-and melanocyte-specific marker, interacts with BAF60A and recruits the BAF complex to enhancer regions of genes encoding the Schwann cell differentiation-specific transcription factors OCT6 and KROX20 to drive differentiation and maturation.…”

Section: Baf Complexes In Neural Developmentmentioning

confidence: 99%

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ATP-dependent chromatin remodeling during mammalian development

2016

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Precise gene expression ensures proper stem and progenitor cell differentiation, lineage commitment and organogenesis during mammalian development. ATP-dependent chromatin-remodeling complexes utilize the energy from ATP hydrolysis to reorganize chromatin and, hence, regulate gene expression. These complexes contain diverse subunits that together provide a multitude of functions, from early embryogenesis through cell differentiation and development into various adult tissues. Here, we review the functions of chromatin remodelers and their different subunits during mammalian development. We discuss the mechanisms by which chromatin remodelers function and highlight their specificities during mammalian cell differentiation and organogenesis.

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Section: Baf Complexes In Neural Developmentsupporting

confidence: 67%

Section: Baf Complexes In Neural Developmentmentioning

confidence: 99%

ATP-dependent chromatin remodeling during mammalian development

2016

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“…However, given the minor effect of in vivo NFkB inactivation on myelination [36], BrG1 interaction with NFkB is likely to have minor functions on SC myelination. Furthermore, while Sox10 levels are moderately [37] or not [38] affected in the absence of BrG1 in SCs, Oct6, Krox20 and P0 are virtually absent. Indeed, the BAF complex is recruited by Sox10 to the Oct6 SCE (SC enhancer [39]), the Krox20 MSE and the P0 promoter to induce Oct6, Krox20 and P0 expression [38][39][40], and thereby controls the myelination process.…”

Section: Hdac1/2 Control Sc Lineage Specificationmentioning

confidence: 92%

“…The BAF complex ATPase BrG1 is required for radial sorting and myelination Ablation of BrG1 in SC precursors (using floxed Brg1 and Dhh-Cre mouse lines) prevents radial sorting and myelination [37,38]. Limpert and colleagues (2013) show that BrG1 interacts with NFkB to activate the Sox10 promoter and suggest that this mechanism controls BrG1-dependent SC 39]), the Krox20 MSE and the P0 promoter to induce Oct6, Krox20 and P0 expression [38][39][40], and thereby controls the myelination process.…”

Section: Hdac1/2 Control Sc Lineage Specificationmentioning

confidence: 99%

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Chromatin-remodeling enzymes in control of Schwann cell development, maintenance and plasticity

Jacob

2017

Current Opinion in Neurobiology

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Gene regulation is essential for cellular differentiation and plasticity. Schwann cells (SCs), the myelinating glia of the peripheral nervous system (PNS), develop from neural crest cells to mature myelinating SCs and can at early developmental stage differentiate into various cell types. After a PNS lesion, SCs can also convert into repair cells that guide and stimulate axonal regrowth, and remyelinate regenerated axons. What controls their development and versatile nature? Several recent studies highlight the key roles of chromatin modifiers in these processes, allowing SCs to regulate their gene expression profile and thereby acquire or change their identity and quickly react to their environment. AddressDepartment of Biology, University of Fribourg, Chemin du Musé e 10, 1700 Fribourg, SwitzerlandCorresponding author: Jacob, Claire (claire.jacob@unifr.ch) IntroductionSCs originate from neural crest cells that also give rise to other cell types including sensory neurons, chondrocytes, melanocytes, smooth-muscle cells [1,2]. After specification in SC precursors, the lineage further differentiates into immature SCs that encircle bundles of axons of different calibers. Next, big caliber axons are sorted in a one-to-one relationship with SCs by a process called radial sorting which leads to the promyelinating stage. The last step of maturation is the myelination process where SCs build a thick myelin sheath rich in lipids around axons (Figure 1). Meanwhile, small caliber axons remain in bundles associated with non-myelinating SCs and persist as Remak bundles in adult nerves [3,4]. Myelin provides axonal insulation and fast conduction of electric signals along axons; its formation and maintenance are thus critical for neuronal functions. By contrast, myelin is detrimental for axonal regrowth after lesion, because it contains growth inhibitory proteins [5]. However, SCs react quickly to an axonal lesion by dedifferentiating, digesting their own myelin -a process called myelinophagy [6] -and converting into repair cells [7,8] that foster axonal regrowth and guide axons back to their former target [9,10]. SCs then remyelinate regenerated axons (Figure 2). This remarkable SC plasticity allows the PNS to functionally regenerate after lesion.This review is focused on the mechanisms of SC development, maintenance and plasticity after lesion controlled by chromatin-remodeling enzymes. Chromatin remodeling regulates the accessibility of genes for the transcriptional machinery, and thereby gene activation and repression. Changes of chromatin architecture are controlled by ATP-dependent nucleosome remodeling and by covalent modifications, either on DNA by methylation or on histones by various post-translational modifications including acetylation, methylation, phosphorylation, ubiquitination, SUMOylation, ADP-ribosylation. Although our knowledge on these mechanisms is still very sparse, recent findings on the functions of chromatinremodeling enzymes have significantly contributed to a better understanding of their critical fu...

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Epigenetic modifications—insight into oligodendrocyte lineage progression, regeneration, and disease

Gregath

2018

FEBS Letters

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Edited by Wilhelm JustMyelination by oligodendrocytes in the central nervous system permits highfidelity saltatory conduction from neuronal cell bodies to axon terminals. Dysmyelinating and demyelinating disorders impair normal nervous system functions. Consequently, an understanding of oligodendrocyte differentiation that moves beyond the genetic code into the field of epigenetics is essential. Chromatin reprogramming is critical for steering stage-specific differentiation processes during oligodendrocyte development. Fine temporal control of chromatin remodeling through ATP-dependent chromatin remodelers and sequential histone modifiers shapes a chromatin regulatory landscape conducive to oligodendrocyte fate specification, lineage differentiation, and maintenance of cell identity. In this Review, we will focus on the biological functions of ATPdependent chromatin remodelers and histone deacetylases in myelinating oligodendrocyte development and implications for myelin regeneration in neurodegenerative diseases.

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Chromatin-Remodeling Factor Brg1 Is Required for Schwann Cell Differentiation and Myelination

Cited by 106 publications

References 36 publications

ATP-dependent chromatin remodeling during mammalian development

ATP-dependent chromatin remodeling during mammalian development

Chromatin-remodeling enzymes in control of Schwann cell development, maintenance and plasticity

Epigenetic modifications—insight into oligodendrocyte lineage progression, regeneration, and disease

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