Glial versus melanocyte cell fate choice: Schwann cell precursors as a cellular origin of melanocytes

Adameyko, Igor; Lallemend, François

doi:10.1007/s00018-010-0390-y

Cited by 54 publications

(43 citation statements)

References 149 publications

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“…At this point, SCPs can be considered as bipotent cells that chose their final fate depending on interactions with the growing nerves. Nerve-derived Neuregulin1 (3,9) or other yet unknown signals could stimulate gliogenesis via Foxd3, a possibility that remains to be tested. In contrast to presumptive SCs, hypaxial melanocytes stemming from the SCP population down-regulate Foxd3 (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…The origins of pigment cells, their ancestral relationship to additional NC derivatives, and the mechanisms by which they segregate from each other remain poorly understood. Research in these areas is of fundamental importance for understanding aspects of pigment cell development as well as of adult physiology and pathology (3).…”

mentioning

confidence: 99%

“…These melanocytes differentiate at late stages relative to pigment cells directly generated from the NC. Thus, in addition to late emigrating/early differentiating NC-derived melanocytes, a subset of early delaminating NC cells that migrate dorsoventrally and later become SCPs in association with the growing nerves can develop either into mature SCs if they remain in contact with nerve fibers or generate melanocytes if they detach from the nerve environment (3,9,10). Except for their common origin from the NC, the relationship between these two melanocyte subsets, at both cellular and molecular levels, remains to be elucidated.…”

mentioning

confidence: 99%

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Neural crest and Schwann cell progenitor-derived melanocytes are two spatially segregated populations similarly regulated by Foxd3

Nitzan

Pfaltzgraff

Labosky

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

103

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Skin melanocytes arise from two sources: either directly from neural crest progenitors or indirectly from neural crest-derived Schwann cell precursors after colonization of peripheral nerves. The relationship between these two melanocyte populations and the factors controlling their specification remains poorly understood. Direct lineage tracing reveals that neural crest and Schwann cell progenitor-derived melanocytes are differentially restricted to the epaxial and hypaxial body domains, respectively. Furthermore, although both populations are initially part of the Foxd3 lineage, hypaxial melanocytes lose Foxd3 at late stages upon separation from the nerve, whereas we recently found that epaxial melanocytes segregate earlier from Foxd3-positive neural progenitors while still residing in the dorsal neural tube. Gain-and loss-offunction experiments in avians and mice, respectively, reveal that Foxd3 is both sufficient and necessary for regulating the balance between melanocyte and Schwann cell development. In addition, Foxd3 is also sufficient to regulate the switch between neuronal and glial fates in sensory ganglia. Together, we propose that differential fate acquisition of neural crest-derived cells depends on their progressive segregation from the Foxd3-positive lineage.

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Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Neural crest and Schwann cell progenitor-derived melanocytes are two spatially segregated populations similarly regulated by Foxd3

Nitzan

Pfaltzgraff

Labosky

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

103

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“…SCPs are believed to be a transient cell population formed during development from NCCs of the ventral migratory pathway in the trunk that can differentiate into Schwann cells. Within the nerves, neuregulin 1 inserted into the axonal membrane of motor and sensory neurons promotes a glial and inhibits a melanocyte fate, whereas insulin-like growth factor (IGF) and platelet-derived growth factor (PDGF) produced by maturing Schwann cells promote a melanocyte fate of SCPs in the nerves (Adameyko and Lallemend, 2010;Adameyko et al, 2009;Ernfors, 2010). However, the origin of melanocytes in the head region has remained unclear.…”

Section: Introductionmentioning

confidence: 99%

Sox2 and Mitf cross-regulatory interactions consolidate progenitor and melanocyte lineages in the cranial neural crest

et al. 2012

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SUMMARYThe cellular origin and molecular mechanisms regulating pigmentation of head and neck are largely unknown. Melanocyte specification is controlled by the transcriptional activity of Mitf, but no general logic has emerged to explain how Mitf and progenitor transcriptional activities consolidate melanocyte and progenitor cell fates. We show that cranial melanocytes arise from at least two different cellular sources: initially from nerve-associated Schwann cell precursors (SCPs) and later from a cellular source that is independent of nerves. Unlike the midbrain-hindbrain cluster from which melanoblasts arise independently of nerves, a large center of melanocytes in and around cranial nerves IX-X is derived from SCPs, as shown by genetic cell-lineage tracing and analysis of ErbB3-null mutant mice. Conditional gain-and loss-of-function experiments show genetically that cell fates in the neural crest involve both the SRY transcription factor Sox2 and Mitf, which consolidate an SCP progenitor or melanocyte fate by cross-regulatory interactions. A gradual downregulation of Sox2 in progenitors during development permits the differentiation of both neural crest-and SCP-derived progenitors into melanocytes, and an initial small pool of nerveassociated melanoblasts expands in number and disperses under the control of endothelin receptor B (Ednrb) and Wnt5a signaling.

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“…Furthermore, attenuating expression of the melanocyte regulator microphtalmia-associated transcription factor (MITF) in culture facilitated the advent of glial markers (Thomas and Erickson, 2008;Thomas and Erickson, 2009). In addition, in vivo analysis showed that a late subset of melanocytes is normally produced from an initial population of Schwann cell precursors (Adameyko et al, 2009), and some diseases of the NC-derived nervous system are frequently associated with abnormal pigmentation (Adameyko and Lallemend, 2010).…”

Section: Introductionmentioning

confidence: 99%

A dynamic code of dorsal neural tube genes regulates the segregation between neurogenic and melanogenic neural crest cells

Nitzan¹,

Krispin²,

Pfaltzgraff

et al. 2013

Development

104

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SUMMARYUnderstanding when and how multipotent progenitors segregate into diverse fates is a key question during embryonic development. The neural crest (NC) is an exemplary model system with which to investigate the dynamics of progenitor cell specification, as it generates a multitude of derivatives. Based on 'in ovo' lineage analysis, we previously suggested an early fate restriction of premigratory trunk NC to generate neural versus melanogenic fates, yet the timing of fate segregation and the underlying mechanisms remained unknown. Analysis of progenitors expressing a Foxd3 reporter reveals that prospective melanoblasts downregulate Foxd3 and have already segregated from neural lineages before emigration. When this downregulation is prevented, late-emigrating avian precursors fail to upregulate the melanogenic markers Mitf and MC/1 and the guidance receptor Ednrb2, generating instead glial cells that express P0 and Fabp. In this context, Foxd3 lies downstream of Snail2 and Sox9, constituting a minimal network upstream of Mitf and Ednrb2 to link melanogenic specification with migration. Consistent with the gain-of-function data in avians, loss of Foxd3 function in mouse NC results in ectopic melanogenesis in the dorsal tube and sensory ganglia. Altogether, Foxd3 is part of a dynamically expressed gene network that is necessary and sufficient to regulate fate decisions in premigratory NC. Their timely downregulation in the dorsal neural tube is thus necessary for the switch between neural and melanocytic phases of NC development.

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Glial versus melanocyte cell fate choice: Schwann cell precursors as a cellular origin of melanocytes

Cited by 54 publications

References 149 publications

Neural crest and Schwann cell progenitor-derived melanocytes are two spatially segregated populations similarly regulated by Foxd3

Neural crest and Schwann cell progenitor-derived melanocytes are two spatially segregated populations similarly regulated by Foxd3

Sox2 and Mitf cross-regulatory interactions consolidate progenitor and melanocyte lineages in the cranial neural crest

A dynamic code of dorsal neural tube genes regulates the segregation between neurogenic and melanogenic neural crest cells

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