Literature DB >> 11874486

Transforming growth factor beta1 regulates melanocyte proliferation and differentiation in mouse neural crest cells via stem cell factor/KIT signaling.

Tamihiro Kawakami1, Yoshinao Soma, Yoko Kawa, Masaru Ito, Emiko Yamasaki, Hidenori Watabe, Eri Hosaka, Kenji Yajima, Kayoko Ohsumi, Masako Mizoguchi.   

Abstract

Stem cell factor is essential to the migration and differentiation of melanocytes during embryogenesis based on the observation that mutations in either the stem cell factor gene, or its ligand, KIT, result in defects in coat pigmentation in mice. Stem cell factor is also required for the survival of melanocyte precursors while they are migrating towards the skin. Transforming growth factor beta1 has been implicated in the regulation of both cellular proliferation and differentiation. NCC-melb4, an immortal cloned cell line, was cloned from a mouse neural crest cell. NCC-melb4 cells provide a model to study the specific stage of differentiation and proliferation of melanocytes. They also express KIT as a melanoblast marker. Using the NCC-melb4 cell line, we investigated the effect of transforming growth factor beta1 on the differentiation and proliferation of immature melanocyte precursors. Immunohistochemically, NCC-melb4 cells showed transforming growth factor beta1 expression. The anti-transforming growth factor beta1 antibody inhibited the cell growth, and downregulated the KIT protein and mRNA expression. To investigate further the activation of autocrine transforming growth factor beta1, NCC-melb4 cells were incubated in nonexogenous transforming growth factor beta1 culture medium. KIT protein decreased with anti-transforming growth factor beta1 antibody concentration in a concentration-dependent manner. We concluded that in NCC-melb4 cells, transforming growth factor beta1 promotes melanocyte precursor proliferation in autocrine and/or paracrine regulation. We further investigated the influence of transforming growth factor beta1 in vitro using a neural crest cell primary culture system from wild-type mice. Anti-transforming growth factor beta1 antibody decreased the number of KIT positive neural crest cell. In addition, the anti-transforming growth factor beta1 antibody supplied within the wild-type neural crest explants abolished the growth of the neural crest cell. These results indicate that transforming growth factor beta1 affect melanocyte precursor proliferation and differentiation in the presence of stem cell factor/KIT in an autocrine/paracrine manner.

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Year:  2002        PMID: 11874486     DOI: 10.1046/j.0022-202x.2001.01696.x

Source DB:  PubMed          Journal:  J Invest Dermatol        ISSN: 0022-202X            Impact factor:   8.551


  6 in total

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Review 3.  Germline mutations of KIT in gastrointestinal stromal tumor (GIST) and mastocytosis.

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Journal:  Cell Biosci       Date:  2016-10-18       Impact factor: 7.133

4.  Paracrine Secreted Frizzled-Related Protein 4 Inhibits Melanocytes Differentiation in Hair Follicle.

Authors:  Haiying Guo; Mingxing Lei; Yuhong Li; Yingxin Liu; Yinhong Tang; Yizhan Xing; Fang Deng; Ke Yang
Journal:  Stem Cells Int       Date:  2017-02-27       Impact factor: 5.443

5.  Single-Cell RNA Sequencing Unravels Heterogeneity of the Stromal Niche in Cutaneous Melanoma Heterogeneous Spheroids.

Authors:  Jiří Novotný; Karolína Strnadová; Barbora Dvořánková; Šárka Kocourková; Radek Jakša; Pavel Dundr; Václav Pačes; Karel Smetana; Michal Kolář; Lukáš Lacina
Journal:  Cancers (Basel)       Date:  2020-11-10       Impact factor: 6.639

6.  Aberrant DNA methylation of GATA binding protein 3 (GATA3), interleukin-4 (IL-4), and transforming growth factor-β (TGF-β) promoters in Behcet's disease.

Authors:  Yunyun Zhu; Yiguo Qiu; Hongsong Yu; Shenglan Yi; Wencheng Su; Aize Kijlstra; Peizeng Yang
Journal:  Oncotarget       Date:  2017-07-22
  6 in total

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