Literature DB >> 16419042

Spatiotemporal gene control by the Cre-ERT2 system in melanocytes.

Ichiro Yajima1, Elodie Belloir, Yveline Bourgeois, Mayuko Kumasaka, Véronique Delmas, Lionel Larue.   

Abstract

The organ-specific and temporal control of gene activation/inactivation is a key issue in the understanding of protein function during normal and pathological development and during oncogenesis. We generated transgenic mice bearing a tamoxifen-dependent Cre recombinase (Tyr::Cre-ERT2) gene expressed under the control of a 6.1 kb murine tyrosinase promoter in order to facilitate targeted spatiotemporally controlled somatic recombination in melanoblasts/melanocytes. Cre-ERT2 production was detected in tissues containing melanocytes. After tamoxifen induction at various times during embryogenesis and adulthood in a Cre-responsive reporter mouse strain, genetic recombination was detected in the melanoblasts and melanocytes of the skin. Thus, the Tyr::Cre-ERT2 transgenic mice provides a valuable tool for following this cell lineage and for investigating gene function in melanocyte development and transformation. (c) 2006 Wiley-Liss, Inc.

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Year:  2006        PMID: 16419042     DOI: 10.1002/gene.20182

Source DB:  PubMed          Journal:  Genesis        ISSN: 1526-954X            Impact factor:   2.487


  27 in total

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7.  Beta-catenin induces immortalization of melanocytes by suppressing p16INK4a expression and cooperates with N-Ras in melanoma development.

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8.  Postnatal lineage mapping of follicular melanocytes with the Tyr::CreER(T) (2) transgene.

Authors:  Melissa L Harris; William J Pavan
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9.  Rac1 drives melanoblast organization during mouse development by orchestrating pseudopod- driven motility and cell-cycle progression.

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Journal:  Nature       Date:  2017-06-28       Impact factor: 49.962

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