Literature DB >> 9272949

Early- and late-migrating cranial neural crest cell populations have equivalent developmental potential in vivo.

C V Baker1, M Bronner-Fraser, N M Le Douarin, M A Teillet.   

Abstract

We present the first in vivo study of the long-term fate and potential of early-migrating and late-migrating mesencephalic neural crest cell populations, by performing isochronic and heterochronic quail-to-chick grafts. Both early- and late-migrating populations form melanocytes, neurons, glia, cartilage and bone in isochronic, isotopic chimeras, showing that neither population is lineage-restricted. The early-migrating population distributes both dorsally and ventrally during normal development, while the late-migrating population is confined dorsally and forms much less cartilage and bone. When the late-migrating population is substituted heterochronically for the early-migrating population, it contributes extensively to ventral derivatives such as jaw cartilage and bone. Conversely, when the early-migrating population is substituted heterochronically for the late-migrating population, it no longer contributes to the jaw skeleton and only forms dorsal derivatives. When the late-migrating population is grafted into a late-stage host whose neural crest had previously been ablated, it migrates ventrally into the jaws. Thus, the dorsal fate restriction of the late-migrating mesencephalic neural crest cell population in normal development is due to the presence of earlier-migrating neural crest cells, rather than to any change in the environment or to any intrinsic difference in migratory ability or potential between early- and late-migrating cell populations. These results highlight the plasticity of the neural crest and show that its fate is determined primarily by the environment.

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Year:  1997        PMID: 9272949     DOI: 10.1242/dev.124.16.3077

Source DB:  PubMed          Journal:  Development        ISSN: 0950-1991            Impact factor:   6.868


  43 in total

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5.  Neural crest invasion is a spatially-ordered progression into the head with higher cell proliferation at the migratory front as revealed by the photoactivatable protein, KikGR.

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Review 8.  Neural crest lineage analysis: from past to future trajectory.

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Review 9.  The molecular basis of neural crest axial identity.

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Review 10.  New perspectives on pharyngeal dorsoventral patterning in development and evolution of the vertebrate jaw.

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Journal:  Dev Biol       Date:  2012-08-30       Impact factor: 3.582

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