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

Jacob, Claire

doi:10.1016/j.conb.2017.08.007

Cited by 33 publications

(36 citation statements)

References 56 publications

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“…This includes the Rac1–MKK7–JNK pathway and mTORC, which elevate c‐Jun and have been implicated as upstream activators of c‐Jun after nerve injury, and the cAMP pathway that suppresses c‐Jun (Arthur‐Farraj et al, ; Monje, Soto, Bacallao, & Wood, ; Norrmén et al, ; Shin et al, ). Histone deacetylase 2 (HDAC2), which is activated in injured nerves, also downregulates c‐Jun (Brügger et al, ; reviewed in Jacob, ). The transcription factors Krox20 and Oct6 also antagonize c‐Jun expression (Brügger et al, ; Parkinson et al, ).…”

Section: Adaptive Cellular Reprogrammingmentioning

confidence: 99%

“…Several epigenetic processes regulate the repair Schwann cell phenotype (Ma & Svaren, ; reviewed in Jacob, ). Injury sets in train chromatin remodeling involving, first, the loss of the active histone mark H3K27 acetylation on enhancers of a number of myelin genes.…”

Section: Adaptive Cellular Reprogrammingmentioning

confidence: 99%

“…Interestingly, macrophage recruitment and Schwann cell numbers, at least at early time points after injury, are less affected in the absence of c-Jun than other aspects of the injury response(Arthur-Farraj et al, 2012). A microarray screening shows that c-Jun controls 172 genes, including directly regulating several neurotrophic factors such as GDNF, BDAF, Shh, and Artemin(Arthur-Farraj et al, 2012;Fontana et al, 2012).However, after nerve injury microarray and RNA-Seq analysis demonstrate at least 4,000-5,000 differentially expressed RNAs, showing that c-Jun only controls a subset of injury induced genes(Arthur- Farraj et al, 2012, 2017Barrette, Calvo, Vallières, & Lacroix, 2010;Bosse, Hasenpusch-Theil, Küry, & Müller, 2006;Chang et al, 2013;Nagarajan, Le, Mahoney, Araki, & Milbrandt, 2002).The extracellular signals that activate Schwann cell c-Jun after injury are obscure. Nevertheless, a number of intracellular pathways that potentially regulate c-Jun levels have been identified.…”

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confidence: 99%

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Repair Schwann cell update: Adaptive reprogramming, EMT, and stemness in regenerating nerves

Jessen

Arthur‐Farraj

2019

Glia

263

260

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Schwann cells respond to nerve injury by cellular reprogramming that generates cells specialized for promoting regeneration and repair. These repair cells clear redundant myelin, attract macrophages, support survival of damaged neurons, encourage axonal growth, and guide axons back to their targets. There are interesting parallels between this response and that found in other tissues. At the cellular level, many other tissues also react to injury by cellular reprogramming, generating cells specialized to promote tissue homeostasis and repair. And at the molecular level, a common feature possessed by Schwann cells and many other cells is the injury‐induced activation of genes associated with epithelial–mesenchymal transitions and stemness, differentiation states that are linked to cellular plasticity and that help injury‐induced tissue remodeling. The number of signaling systems regulating Schwann cell plasticity is rapidly increasing. Importantly, this includes mechanisms that are crucial for the generation of functional repair Schwann cells and nerve regeneration, although they have no or a minor role elsewhere in the Schwann cell lineage. This encourages the view that selective tools can be developed to control these particular cells, amplify their repair supportive functions and prevent their deterioration. In this review, we discuss the emerging similarities between the injury response seen in nerves and in other tissues and survey the transcription factors, epigenetic mechanisms, and signaling cascades that control repair Schwann cells, with emphasis on systems that selectively regulate the Schwann cell injury response.

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Section: Adaptive Cellular Reprogrammingmentioning

confidence: 99%

Section: Adaptive Cellular Reprogrammingmentioning

confidence: 99%

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confidence: 99%

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Repair Schwann cell update: Adaptive reprogramming, EMT, and stemness in regenerating nerves

Jessen

Arthur‐Farraj

2019

Glia

263

260

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“…These have been catalogued in several recent reviews (Küspert & Wegner, ; Stolt & Wegner, ; Svaren & Meijer, ). Similarly, chromatin modifying activities and regulatory RNAs have been identified as important regulators in both types of myelinating glia (Gregath & Lu, ; Jacob, ; Svaren, ). In this review, we will concentrate on transcription factors and put the focus on the functional interactions within their networks.…”

Section: Introductionmentioning

confidence: 99%

Transcriptional control of myelination and remyelination

Sock

Wegner

2019

Glia

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Myelination is an evolutionary recent differentiation program that has been independently acquired in vertebrates by Schwann cells in the peripheral nervous system and oligodendrocytes in the central nervous system. Therefore, it is not surprising that regulating transcription factors differ substantially between both cell types. However, overall principles are similar as transcriptional control in Schwann cells and oligodendrocytes combines lineage determining and stage‐specific factors in complex regulatory networks. Myelination does not only occur during development, but also as remyelination in the adult. In line with the different conditions during developmental myelination and remyelination and the distinctive properties of Schwann cells and oligodendrocytes, transcriptional regulation of remyelination exhibits unique features and differs between the two cell types. This review gives an overview of the current state in the field.

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“…It has become clear that epigenomic changes are important for such reprogramming events, employing mechanisms of gene activation and derepression (Brügger et al 2017; He et al 2018; Hung et al 2015; Jacob 2017; Ma and Svaren 2018). Our previous studies identified the association of trimethylation at Lys27 of histone H3 tail (H3K27me3) at promoters of many genes that become activated after peripheral nerve injury, and we found that the demethylation is required for full activation of some repair genes (Ma et al 2016).…”

Section: Introductionmentioning

confidence: 99%

Polycomb repression regulates Schwann cell proliferation and axon regeneration after nerve injury

Duong

Moran

et al. 2018

Glia

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The transition of differentiated Schwann cells to support of nerve repair after injury is accompanied by remodeling of the Schwann cell epigenome. The EED-containing polycomb repressive complex 2 (PRC2) catalyzes histone H3K27 methylation and represses key nerve repair genes such as Shh, Gdnf and Bdnf, and their activation is accompanied by loss of H3K27 methylation. Analysis of nerve injury in mice with a Schwann cell-specific loss of EED showed the reversal of polycomb repression is required and a rate limiting step in the increased transcription of Neuregulin 1 (type I), which is required for efficient remyelination. However, mouse nerves with EED-deficient Schwann cells display slow axonal regeneration with significantly low expression of axon guidance genes, including Sema4f and Cntf. Finally, EED loss causes impaired Schwann cell proliferation after injury with significant induction of the Cdkn2a cell cycle inhibitor gene. Interestingly, PRC2 subunits and CDKN2A are commonly co-mutated in the transition from benign neurofibromas to malignant peripheral nerve sheath tumors (MPNST’s). RNA-seq analysis of EED-deficient mice identified PRC2-regulated molecular pathways that may contribute to the transition to malignancy in neurofibromatosis.

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

Cited by 33 publications

References 56 publications

Repair Schwann cell update: Adaptive reprogramming, EMT, and stemness in regenerating nerves

Repair Schwann cell update: Adaptive reprogramming, EMT, and stemness in regenerating nerves

Transcriptional control of myelination and remyelination

Polycomb repression regulates Schwann cell proliferation and axon regeneration after nerve injury

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