Akt-Mediated Survival of Oligodendrocytes Induced by Neuregulins

Flores, Ana I.; Mallon, Barbara S.; Mizutani, Takashi; Ogawa, Wataru; Rosenzweig, Anthony; Okamoto, Takashi; Macklin, Wendy B.

doi:10.1523/jneurosci.20-20-07622.2000

Cited by 173 publications

(152 citation statements)

References 74 publications

(79 reference statements)

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“…In this respect, our results are in agreement with previously identified roles of S1P in Akt activation and survival of hepatic myofibroblast or endothelial cells (Morales-Ruiz et al, 2001;Davaille et al, 2002). A variety of different agents have been shown to promote oligodendrocyte survival, and some such as NT3, IGF-I, and neuregulin (Vemuri and McMorris, 1996;Flores et al, 2000) signal through the phosphatidylinositol 3Ј-kinase (PI3K) transduction pathway. S1P therefore appears to be another oligodendroglial survival factor, signaling through the Akt pathway downstream of the Edg8/S1P5 receptor.…”

Section: S1p and Survival Of Mature Oligodendrocytessupporting

confidence: 92%

“…9A). Because the Akt signaling cascade has been previously shown to be involved in oligodendrocyte survival (Vemuri and McMorris, 1996;Flores et al, 2000), we performed an immunoblot with an anti-phosphoAkt mAb on S1P-treated cell extracts from mature oligodendrocytes. Exposure of mature oligodendrocytes to S1P for 15 min induced a robust phosphorylation of Akt, which was mainly prevented by incubation of the cells with PTX (Fig.…”

Section: S1p-induced Survival Of Mature Oligodendrocytes Is Mediated mentioning

confidence: 99%

“…These developmental stages, which are associated with different capacities of proliferation, migration, differentiation, survival, maturation, and finally myelin deposition, are cell autonomous but also depend on a variety of extrinsic factors. Growth factors (PDGF-A, FGF-2, IGF-I, CNTF, neuregulins, and neurotrophins) have been shown to affect proliferation, survival, and differentiation of oligodendrocyte precursor cells (OPCs) (Barres et al, 1992;Bansal and Pfeiffer, 1997;Flores et al, 2000;Sim et al, 2002). Guidance molecules, such as semaphorins 3A, 3F, and netrin-1, guide the migration of OPCs during development (Sugimoto et al, 2001;Spassky et al, 2002;Tsai and Miller, 2002;Jarjour et al, 2003).…”

Section: Introductionmentioning

confidence: 99%

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Edg8/S1P5: An Oligodendroglial Receptor with Dual Function on Process Retraction and Cell Survival

Jaillard

Harrison²,

Stankoff³

et al. 2005

J. Neurosci.

308

273

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Endothelial differentiation gene (Edg) proteins are G-protein-coupled receptors activated by lysophospholipid mediators: sphingosine-1-phosphate (S1P) or lysophosphatidic acid. We show that in the CNS, expression of Edg8/S1P5, a high-affinity S1P receptor, is restricted to oligodendrocytes and expressed throughout development from the immature stages to the mature myelin-forming cell. S1P activation of Edg8/S1P5 on O4-positive pre-oligodendrocytes induced process retraction via a Rho kinase/collapsin response-mediated protein signaling pathway, whereas no retraction was elicited by S1P on these cells derived from Edg8/S1P5-deficient mice. Edg8/S1P5-mediated process retraction was restricted to immature cells and was no longer observed at later developmental stages. In contrast, S1P activation promoted the survival of mature oligodendrocytes but not of pre-oligodendrocytes. The S1P-induced survival of mature oligodendrocytes was mediated through a pertussis toxin-sensitive, Akt-dependent pathway. Our data demonstrate that Edg8/S1P5 activation on oligodendroglial cells modulates two distinct functional pathways mediating either process retraction or cell survival and that these effects depend on the developmental stage of the cell.

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Section: S1p and Survival Of Mature Oligodendrocytessupporting

confidence: 92%

Section: S1p-induced Survival Of Mature Oligodendrocytes Is Mediated mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Edg8/S1P5: An Oligodendroglial Receptor with Dual Function on Process Retraction and Cell Survival

Jaillard

Harrison²,

Stankoff³

et al. 2005

J. Neurosci.

308

273

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“…Akt (also known as protein kinase B) is a serine/threonine protein kinase that transduces intracellular anti-apoptotic signals that are mediated by serum or growth factors that activate phosphoinositide 3-kinase, or PI3-kinase (Franke et al, 1995;Datta et al, 1997;Dudek et al, 1997;Kennedy et al, 1997;Coffer et al, 1998;Downward 1998;Nunez and del Peso, 1998;Goswami et al, 1999;Kennedy et al, 1999;Flores et al, 2000). Overexpression of Akt prevents apoptosis in certain cells, including neurons, following withdrawal of serum or growth factors (Yao and Cooper, 1995;Datta et al, 1997;Dudek et al, 1997;Crowder and Freeman, 1998;Eves et al, 1998;Ulrich et al, 1998;Bhave et al, 1999;Vaillant et al, 1999;Virdee et al, 1999;Flores et al, 2000;Kermer et al, 2000). The precise mechanisms by which Akt promotes cell survival are not entirely clear.…”

Section: Therapeutic Interventions: Delivery Of Anti-apoptotic Genes mentioning

confidence: 99%

Apoptotic Cell Death Following Traumatic Injury to the Central Nervous System

Springer¹

2002

BMB Reports

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Apoptotic cell death is a fundamental and highly regulated biological process in which a cell is instructed to actively participate in its own demise. This process of cellular suicide is activated by developmental and environmental cues and normally plays an essential role in eliminating superfluous, damaged, and senescent cells of many tissue types. In recent years, a number of experimental studies have provided evidence of widespread neuronal and glial apoptosis following injury to the central nervous system (CNS). These studies indicate that injury-induced apoptosis can be detected from hours to days following injury and may contribute to neurological dysfunction. Given these findings, understanding the biochemical signaling events controlling apoptosis is a first step towards developing therapeutic agents that target this cell death process. This review will focus on molecular cell death pathways that are responsible for generating the apoptotic phenotype. It will also summarize what is currently known about the apoptotic signals that are activated in the injured CNS, and what potential strategies might be pursued to reduce this cell death process as a means to promote functional recovery.

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“…This most likely stems from lowered association of the receptor with DRMs in ASA Ϫ/Ϫ NPs. Interestingly, the survival/expansion of OPC mediated by PDGF-AA involves the activation of AKT through phosphorylation of residues Thr 308 and Ser 473 (68,69). Our results demonstrate that in the presence of high levels of sulfatides, the relocalization of PDGFR␣ to non-DRM domains and phosphorylation of Thr 308 and Ser 473 of AKT are severely compromised.…”

Section: Discussionmentioning

confidence: 74%

Dysfunction of Platelet-derived Growth Factor Receptor α (PDGFRα) Represses the Production of Oligodendrocytes from Arylsulfatase A-deficient Multipotential Neural Precursor Cells

Pituch

Moyano

Lopez-Rosas

et al. 2015

Journal of Biological Chemistry

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Background: PDGFR␣ is a key signaling component in oligodendrogenesis. Results: Multipotential Neural precursors (NPs) deficient in arylsulfatase A (ASA) show a higher ratio of long versus short fatty acid sulfatides, reduction in PDGFR␣, decreased AKT phosphorylation, and increased exosomal shedding of PDGFR␣. Conclusion: Sulfatides are regulators of NP response to PDGF-AA. Significance: A novel regulatory mechanism of PDGFR␣ signaling is described.

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Akt-Mediated Survival of Oligodendrocytes Induced by Neuregulins

Cited by 173 publications

References 74 publications

Edg8/S1P5: An Oligodendroglial Receptor with Dual Function on Process Retraction and Cell Survival

Edg8/S1P5: An Oligodendroglial Receptor with Dual Function on Process Retraction and Cell Survival

Apoptotic Cell Death Following Traumatic Injury to the Central Nervous System

Dysfunction of Platelet-derived Growth Factor Receptor α (PDGFRα) Represses the Production of Oligodendrocytes from Arylsulfatase A-deficient Multipotential Neural Precursor Cells

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