Literature DB >> 7619726

Mutations at the W locus affect survival of neural crest-derived melanocytes in the mouse.

J Cable1, I J Jackson, K P Steel.   

Abstract

The development of melanoblasts in normally pigmented and dominant spotting (W) embryos was followed by in situ hybridisation to TRP-2/DT mRNA, which labels migratory melanoblasts from 10 days post coitum. Numerous melanoblasts migrate to the inner ear around 11 days. In contrast, few migratory melanoblasts are associated with the eye or skin at this stage and melanoblasts distribution within the trunk and tail is patchy. The distribution of melanoblasts in 10.5-11-day-old Wv/Wv, Wsh/Wsh and W41/W41 mutants was similar to that in controls but melanoblasts density was lower and by 12 days was severely reduced. These results suggest that mutations of the c-kit receptor tyrosine kinase encoded at the W locus do not alter early migration or differentiation of melanoblasts but severely affect melanoblasts survival.

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Year:  1995        PMID: 7619726     DOI: 10.1016/0925-4773(94)00331-g

Source DB:  PubMed          Journal:  Mech Dev        ISSN: 0925-4773            Impact factor:   1.882


  40 in total

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Review 5.  Aging, graying and loss of melanocyte stem cells.

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6.  Sooty foot, a novel mouse mutation that affects the pigmentation of exposed skin, but not hair, maps to chromosome 2.

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Review 7.  Receptor tyrosine kinase signaling: regulating neural crest development one phosphate at a time.

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Authors:  Margaret G Mills; Larissa B Patterson
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9.  The c-kit signaling pathway is involved in the development of persistent pain.

Authors:  Yan-Gang Sun; Neilia G Gracias; Julie Kosto Drobish; Michael R Vasko; Robert W Gereau; Zhou-Feng Chen
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10.  Differentiation of zebrafish melanophores depends on transcription factors AP2 alpha and AP2 epsilon.

Authors:  Eric Van Otterloo; Wei Li; Gregory Bonde; Kristopher M Day; Mei-Yu Hsu; Robert A Cornell
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