Reduced EGFR signaling in progenitor cells of the adult subventricular zone attenuates oligodendrogenesis after demyelination

Aguirre, Adán; Gallo, Vittorio

doi:10.1017/s1740925x08000082

Cited by 71 publications

(64 citation statements)

References 54 publications

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“…1d,e). We have previously demonstrated that in the 2′,3′-cyclic-nucleotide 3′-phosphodiesterase (CNP)-EGFP mouse, in which all developmental stages of the OL lineage can be visualized based on EGFP expression, the majority of proliferating EGFP + cells under normal or pathological conditions are OPCs1435. Therefore, we wanted to determine whether Sirt1 expression was upregulated in proliferative OPCs.…”

Section: Resultsmentioning

confidence: 99%

“…To determine whether Sirt1 plays a specific role in OPC proliferation in neonatal white matter, we used a model of focal (lysolecithin-induced) demyelination of adult white matter35. We analysed white matter lesions at 7 days after demyelination, that is, at a time point when OPC proliferation is maximal35.…”

Section: Resultsmentioning

confidence: 99%

“…We analysed white matter lesions at 7 days after demyelination, that is, at a time point when OPC proliferation is maximal35. Differently from neonatal HX, focal demyelination led to a reduction of Sirt1 + and Sirt1 + BrdU + cells in the adult white matter (Supplementary Fig.…”

Section: Resultsmentioning

confidence: 99%

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Sirt1 regulates glial progenitor proliferation and regeneration in white matter after neonatal brain injury

et al. 2016

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Regenerative processes in brain pathologies require the production of distinct neural cell populations from endogenous progenitor cells. We have previously demonstrated that oligodendrocyte progenitor cell (OPC) proliferation is crucial for oligodendrocyte (OL) regeneration in a mouse model of neonatal hypoxia (HX) that reproduces diffuse white matter injury (DWMI) of premature infants. Here we identify the histone deacetylase Sirt1 as a Cdk2 regulator in OPC proliferation and response to HX. HX enhances Sirt1 and Sirt1/Cdk2 complex formation through HIF1α activation. Sirt1 deacetylates retinoblastoma (Rb) in the Rb/E2F1 complex, leading to dissociation of E2F1 and enhanced OPC proliferation. Sirt1 knockdown in culture and its targeted ablation in vivo suppresses basal and HX-induced OPC proliferation. Inhibition of Sirt1 also promotes OPC differentiation after HX. Our results indicate that Sirt1 is an essential regulator of OPC proliferation and OL regeneration after neonatal brain injury. Therefore, enhancing Sirt1 activity may promote OL recovery after DWMI.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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Sirt1 regulates glial progenitor proliferation and regeneration in white matter after neonatal brain injury

et al. 2016

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“…Accordingly, mutant mice defective in TGFα or EGFR expression present reduced numbers of astrocytes at the adult age (Kornblum et al 1998 ;Sibilia et al 1998 ;Weickert and Blum 1995 ) and enhanced astrocyte apoptosis (Wagner et al 2006 ). Like astrocytes, NSC and NPC (including the NG2 progenitor population) remain responsive to EGFR signaling from development to adult ages, responding notably to EGFR activation by enhanced proliferation (Aguirre and Gallo 2007 ;Craig et al 1996 ;Doetsch et al 2002 ; ( a ) Schematic representation of the signaling pathways most frequently deregulated in human glioma. Genes whose activation or inhibition is associated with glioma are depicted in rose and blue, respectively.…”

Section: Common Signalling Pathways Controlling Gliosis and Glioma Dementioning

confidence: 99%

Links Between Injury-Induced Brain Remodeling and Oncogenesis

El-Habr

Junier

2014

Endogenous Stem Cell-Based Brain Remodeling in Mammals

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“…EGF was increased in the injured region of the cortex to which SVZ cells migrated after cortical aspiration [202], while cerebral ischemia produced a larger number of EGFR-positive NPCs in the SVZ [20,203]. Following nigrostriatal denervation, TGFα infusion into the striatum induced emigration of SVZ cells [204,205], while reduction of EGFR signaling in progenitors expressing neuron glial antigen 2 decreased their proliferative and migratory response to demyelination [206]. Interestingly, Ninomiya et al [203] showed that in the ischemic brain there was an increase in the number of NPCs but a decrease in neuroblasts during EGF infusion into the parenchyma; however, 6 days after the discontinuation of EGF delivery, there was a substantial rise in the number of neuroblasts in the SVZ and striatum.…”

Section: Injury-induced Factors Mediating Redirected Migration To Dammentioning

confidence: 99%

Inflammatory Regulators of Redirected Neural Migration in the Injured Brain

2012

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Reduced EGFR signaling in progenitor cells of the adult subventricular zone attenuates oligodendrogenesis after demyelination

Cited by 71 publications

References 54 publications

Sirt1 regulates glial progenitor proliferation and regeneration in white matter after neonatal brain injury

Sirt1 regulates glial progenitor proliferation and regeneration in white matter after neonatal brain injury

Links Between Injury-Induced Brain Remodeling and Oncogenesis

Inflammatory Regulators of Redirected Neural Migration in the Injured Brain

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