<i>notch3</i>is essential for oligodendrocyte development and vascular integrity in zebrafish

Zaucker, Andreas; Mercurio, Sara; Sternheim, Nitzan; Talbot, William S.; Marlow, Florence

doi:10.1242/dmm.012005

Cited by 32 publications

(44 citation statements)

References 91 publications

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“…S4A), whereas only notch3 fh332 mutant embryos exhibited cranial hemorrhage (supplementary material Fig. S4A), as recently reported (Wang et al, 2014;Zaucker et al, 2013). We also noted increased numbers of ISV endothelial cells only in embryos deficient for notch1b (supplementary material Fig.…”

Section: Multiple Notch Receptors and Ligands Contribute To Artery DIsupporting

confidence: 87%

“…Although combining genetic manipulation of Notch signaling with the tp1-driven transgenes has been helpful, generation of receptor-specific sensors, similar to NIP-Cre, or Gal4 fusions used successfully in Drosophila (Struhl and Adachi, 1998), will be needed moving forward. jh15 nred) jh15 ], notch1a tp37 , deltac tit446 , dll4 j16e1 and notch3 fh332 have been described elsewhere (Clements et al, 2011;Covassin et al, 2009;Holley et al, 2002;Jülich et al, 2005;Leslie et al, 2007;Parsons et al, 2009;Zaucker et al, 2013). Lines generated in this study are described below.…”

Section: Discussionmentioning

confidence: 99%

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Distinct Notch signaling outputs pattern the developing arterial system

et al. 2014

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Differentiation of arteries and veins is essential for the development of a functional circulatory system. In vertebrate embryos, genetic manipulation of Notch signaling has demonstrated the importance of this pathway in driving artery endothelial cell differentiation. However, when and where Notch activation occurs to affect endothelial cell fate is less clear. Using transgenic zebrafish bearing a Notch-responsive reporter, we demonstrate that Notch is activated in endothelial progenitors during vasculogenesis prior to blood vessel morphogenesis and is maintained in arterial endothelial cells throughout larval stages. Furthermore, we find that endothelial progenitors in which Notch is activated are committed to a dorsal aorta fate. Interestingly, some arterial endothelial cells subsequently downregulate Notch signaling and then contribute to veins during vascular remodeling. Lineage analysis, together with perturbation of both Notch receptor and ligand function, further suggests several distinct developmental windows in which Notch signaling acts to promote artery commitment and maintenance. Together, these findings demonstrate that Notch acts in distinct contexts to initiate and maintain artery identity during embryogenesis.

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Section: Multiple Notch Receptors and Ligands Contribute To Artery DIsupporting

confidence: 87%

Section: Discussionmentioning

confidence: 99%

Distinct Notch signaling outputs pattern the developing arterial system

et al. 2014

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“…Therefore, the small number of pericytes that develop in notch3 fh332 mutants is not sufficient to direct BBB formation, indicating that Notch3 function is part of a mechanism to promote adequate pericyte coverage of brain vessels. Notably, a recent study using independently identified notch3 hypomorphic alleles suggested that reduced Notch3 signaling compromised vascular tone and vascular integrity in the fins of adult zebrafish (Zaucker et al, 2013). Mural cells could not be unambiguously identified in the fin vasculature of notch3 mutants, supporting our own results.…”

Section: Research Articlesupporting

confidence: 70%

Notch3 establishes brain vascular integrity by regulating pericyte number

et al. 2014

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Brain pericytes are important regulators of brain vascular integrity, permeability and blood flow. Deficiencies of brain pericytes are associated with neonatal intracranial hemorrhage in human fetuses, as well as stroke and neurodegeneration in adults. Despite the important functions of brain pericytes, the mechanisms underlying their development are not well understood and little is known about how pericyte density is regulated across the brain. The Notch signaling pathway has been implicated in pericyte development, but its exact roles remain ill defined. Here, we report an investigation of the Notch3 receptor using zebrafish as a model system. We show that zebrafish brain pericytes express notch3 and that notch3 mutant zebrafish have a deficit of brain pericytes and impaired blood-brain barrier function. Conditional loss-and gain-of-function experiments provide evidence that Notch3 signaling positively regulates brain pericyte proliferation. These findings establish a new role for Notch signaling in brain vascular development whereby Notch3 signaling promotes expansion of the brain pericyte population.

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“…43 Another study showed that Notch3 regulates OPC development and myelin basic protein gene and maintains vascular integrity using zebrafish notch3 mutants. 44 Notch3 may have corresponding roles in OPC development and in encouraging vascular integrity, and also, there is a possibility that notch3 might comprise the communication between OPC and vascular cell. 44 …”

Section: Transgenic Mouse Lines For Cerebral Autosomal Dominant Artermentioning

confidence: 99%

“…44 Notch3 may have corresponding roles in OPC development and in encouraging vascular integrity, and also, there is a possibility that notch3 might comprise the communication between OPC and vascular cell. 44 …”

Section: Transgenic Mouse Lines For Cerebral Autosomal Dominant Artermentioning

confidence: 99%

Subcortical ischemic vascular disease: Roles of oligodendrocyte function in experimental models of subcortical white-matter injury

Shindo

Liang

Maki

et al. 2015

J Cereb Blood Flow Metab

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Oligodendrocytes are one of the major cell types in cerebral white matter. Under normal conditions, they form myelin sheaths that encircle axons to support fast nerve conduction. Under conditions of cerebral ischemia, oligodendrocytes tend to die, resulting in white-matter dysfunction. Repair of white matter involves the ability of oligodendrocyte precursors to proliferate and mature. However, replacement of lost oligodendrocytes may not be the only mechanism for white-matter recovery. Emerging data now suggest that coordinated signaling between neural, glial, and vascular cells in the entire neurovascular unit may be required. In this mini-review, we discuss how oligodendrocyte lineage cells participate in signaling and crosstalk with other cell types to underlie function and recovery in various experimental models of subcortical white-matter injury.

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notch3is essential for oligodendrocyte development and vascular integrity in zebrafish

Cited by 32 publications

References 91 publications

Distinct Notch signaling outputs pattern the developing arterial system

Distinct Notch signaling outputs pattern the developing arterial system

Notch3 establishes brain vascular integrity by regulating pericyte number

Subcortical ischemic vascular disease: Roles of oligodendrocyte function in experimental models of subcortical white-matter injury

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