Sulfatase 1 Promotes the Motor Neuron-to-Oligodendrocyte Fate Switch by Activating Shh Signaling in Olig2 Progenitors of the Embryonic Ventral Spinal Cord

Touahri, Yacine; Escalas, Nathalie; Bénazéraf, Bertrand; Cochard, Philippe; Danesin, Cathy; Soula, Cathy

doi:10.1523/jneurosci.3553-12.2012

Cited by 47 publications

(95 citation statements)

References 84 publications

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“…Strikingly, this neuroglial switch is also controlled by Shh, responsible at that time for a rearrangement of the ventral patterning, resulting in generation of the p* domain. This domain forms following dorsal expansion of Nkx2.2 expression in Olig2 progenitors in response to a rise in Shh signaling Danesin et al, 2006;Fu et al, 2002;Touahri et al, 2012;Zhou et al, 2001). At this stage, Nkx2.2 no longer represses Olig2 and their co-expression drives p* progenitors to the OPC fate.…”

Section: Introductionmentioning

confidence: 99%

“…At this stage, Nkx2.2 no longer represses Olig2 and their co-expression drives p* progenitors to the OPC fate. We identified the secreted enzyme Sulfatase1 (Sulf1) as a major player in triggering this cell fate change in amniotes (Touahri et al, 2012). By modulating the sulfation state of heparan sulphate proteoglycans (HSPGs) at the cell surface, Sulf1 regulates interaction of HSPGs with morphogen factors (Ai et al, 2003;Dhoot et al, 2001;Freeman et al, 2008;Lamanna et al, 2007;Meyers et al, 2013;Viviano et al, 2004;Wang et al, 2004).…”

Section: Introductionmentioning

confidence: 99%

“…In Drosophila, Sulf1 has opposing functions, enhancing Hh release from its source and reducing Hh signaling activity in the responding cells (Wojcinski et al, 2011). In vertebrate spinal cord, Sulf1 only behaves as a positive modulator of Shh signaling (Danesin et al, 2006;Touahri et al, 2012). Strikingly, the expression of Sulf1 is highly dynamic in this tissue.…”

Section: Introductionmentioning

confidence: 99%

“…Strikingly, the expression of Sulf1 is highly dynamic in this tissue. Its function in triggering the MN/OPC fate switch is related to its upregulation in Nkx2.2 progenitors (Braquart-Varnier et al, 2004;Danesin et al, 2006;Touahri et al, 2012), suggesting that Sulf1, by lowering the Shh-HSPG interaction at the surface of p3 progenitors, helps to provide higher doses of Shh, free to travel dorsally, to Olig2 progenitors. However, the mechanism by which Sulf1 non-cell autonomously activates Shh signaling has yet to be elucidated.…”

Section: Introductionmentioning

confidence: 99%

“…Before patterning rearrangement, Sulf1 is expressed in the ventral neural tube (Braquart-Varnier et al, 2004;Danesin et al, 2006;Gorsi et al, 2010;Meyers et al, 2013;Touahri et al, 2012), opening the possibility that it could also influence Shh signaling at stages of patterning establishment. We report that, in addition to its function in stimulating OPC induction, Sulf1 activity is crucial for generation of ventral neuronal subtypes in zebrafish.…”

Section: Introductionmentioning

confidence: 99%

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Dynamics of Sonic hedgehog signaling in the ventral spinal cord are controlled by intrinsic changes in source cells requiring Sulfatase 1

et al. 2014

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In the ventral spinal cord, generation of neuronal and glial cell subtypes is controlled by Sonic hedgehog (Shh). This morphogen contributes to cell diversity by regulating spatial and temporal sequences of gene expression during development. Here, we report that establishing Shh source cells is not sufficient to induce the highthreshold response required to specify sequential generation of ventral interneurons and oligodendroglial cells at the right time and place in zebrafish. Instead, we show that Shh-producing cells must repeatedly upregulate the secreted enzyme Sulfatase1 (Sulf1) at two critical time points of development to reach their full inductive capacity. We provide evidence that Sulf1 triggers Shh signaling activity to establish and, later on, modify the spatial arrangement of gene expression in ventral neural progenitors. We further present arguments in favor of Sulf1 controlling Shh temporal activity by stimulating production of active forms of Shh from its source. Our work, by pointing out the key role of Sulf1 in regulating Shhdependent neural cell diversity, highlights a novel level of regulation, which involves temporal evolution of Shh source properties.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Dynamics of Sonic hedgehog signaling in the ventral spinal cord are controlled by intrinsic changes in source cells requiring Sulfatase 1

et al. 2014

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Oligodendrocyte generation during mouse development

Takebayashi

Ikenaka

2015

Glia

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Oligodendrocytes (OLs) are glial cells, which generate myelin in the central nervous system. Their interesting developmental features attract many neurobiologists eager to study cell differentiation, gene expression regulation, or dynamic morphogenesis. Their primary role in protecting the axons has major impacts in the medical research field: in multiple sclerosis, a demyelinating disease in which remyelination is blocked. Oligodendrogenesis is involved in higher brain function including motor skill learning and cognitive function. Here, we review advances in the research on OL development and highlight areas where questions remain to be answered in both developmental biology and neurobiology related aspects.

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Sulfatase 2 promotes generation of a spinal cord astrocyte subtype that stands out through the expression of Olig2

Ohayon

Escalas

Cochard

et al. 2019

Glia

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Generation of glial cell diversity in the developing spinal cord is known to depend on spatio‐temporal patterning programs. In particular, expression of the transcription factor Olig2 in neural progenitors of the pMN domain is recognized as critical to their fate choice decision to form oligodendrocyte precursor cells (OPCs) instead of astrocyte precursors (APs). However, generating some confusion, lineage‐tracing studies of Olig2 progenitors in the spinal cord provided evidence that these progenitors also generate some astrocytes. Here, we addressed the role of the heparan sulfate‐editing enzyme Sulf2 in the control of gliogenesis and found an unanticipated function for this enzyme. At initiation of gliogenesis in mouse, Sulf2 is expressed in ventral neural progenitors of the embryonic spinal cord, including in Olig2‐expressing cells of the pMN domain. We found that sulf2 deletion, while not affecting OPC production, impairs generation of a previously unknown Olig2‐expressing pMN‐derived cell subtype that, in contrast to OPCs, does not upregulate Sox10, PDGFRα or Olig1. Instead, these cells activate expression of AP identity genes, including aldh1L1 and fgfr3 and, of note, retain Olig2 expression as they populate the spinal parenchyma at embryonic stages but also as they differentiate into mature astrocytes at postnatal stages. Thus, our study, by revealing the existence of Olig2‐expressing APs that segregate early from pMN cells under the influence of Sulf2, supports the existence of a common source of APs and OPCs in the ventral spinal cord and highlights divergent regulatory mechanism for the development of pMN‐derived OPCs and APs.

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Sulfatase 1 Promotes the Motor Neuron-to-Oligodendrocyte Fate Switch by Activating Shh Signaling in Olig2 Progenitors of the Embryonic Ventral Spinal Cord

Cited by 47 publications

References 84 publications

Dynamics of Sonic hedgehog signaling in the ventral spinal cord are controlled by intrinsic changes in source cells requiring Sulfatase 1

Dynamics of Sonic hedgehog signaling in the ventral spinal cord are controlled by intrinsic changes in source cells requiring Sulfatase 1

Oligodendrocyte generation during mouse development

Sulfatase 2 promotes generation of a spinal cord astrocyte subtype that stands out through the expression of Olig2

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