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β-连环蛋白的稳定促进了黑素细胞的特化,而牺牲了施万细胞谱系。

Stabilization of β-catenin promotes melanocyte specification at the expense of the Schwann cell lineage.

机构信息

Institut Curie, PSL Research University, INSERM U1021, Normal and Pathological Development of Melanocytes, Orsay, France.

Univ Paris-Sud, Univ Paris-Saclay, CNRS UMR 3347, Orsay, France.

出版信息

Development. 2022 Jan 15;149(2). doi: 10.1242/dev.194407. Epub 2022 Jan 24.

DOI:10.1242/dev.194407
PMID:34878101
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8917410/
Abstract

The canonical Wnt/β-catenin pathway governs a multitude of developmental processes in various cell lineages, including the melanocyte lineage. Indeed, β-catenin regulates transcription of Mitf-M, the master regulator of this lineage. The first wave of melanocytes to colonize the skin is directly derived from neural crest cells, whereas the second wave of melanocytes is derived from Schwann cell precursors (SCPs). We investigated the influence of β-catenin in the development of melanocytes of the first and second waves by generating mice expressing a constitutively active form of β-catenin in cells expressing tyrosinase. Constitutive activation of β-catenin did not affect the development of truncal melanoblasts but led to marked hyperpigmentation of the paws. By activating β-catenin at various stages of development (E8.5-E11.5), we showed that the activation of β-catenin in bipotent SCPs favored melanoblast specification at the expense of Schwann cells in the limbs within a specific temporal window. Furthermore, in vitro hyperactivation of the Wnt/β-catenin pathway, which is required for melanocyte development, induces activation of Mitf-M, in turn repressing FoxD3 expression. In conclusion, β-catenin overexpression promotes SCP cell fate decisions towards the melanocyte lineage.

摘要

经典的 Wnt/β-连环蛋白途径调控着各种细胞谱系中的多种发育过程,包括黑素细胞谱系。事实上,β-连环蛋白调节着该谱系的主调控因子 Mitf-M 的转录。首先,一批黑素细胞直接来源于神经嵴细胞,而第二批黑素细胞则来源于许旺细胞前体(SCPs)。我们通过在表达酪氨酸酶的细胞中表达组成型激活形式的β-连环蛋白,研究了β-连环蛋白对第一波和第二波黑素细胞发育的影响。β-连环蛋白的组成型激活并不影响躯干黑素母细胞的发育,但导致爪子明显色素沉着过度。通过在发育的各个阶段(E8.5-E11.5)激活β-连环蛋白,我们表明,在特定的时间窗口内,在多能性 SCPs 中激活β-连环蛋白有利于黑素细胞的特化,而牺牲了四肢中的许旺细胞。此外,体外对 Wnt/β-连环蛋白途径的过度激活,这是黑素细胞发育所必需的,诱导了 Mitf-M 的激活,进而抑制了 FoxD3 的表达。总之,β-连环蛋白过表达促进了 SCP 细胞命运决定向黑素细胞谱系的方向发展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/89b7/8917410/e76cb3cc9aef/develop-149-194407-g8.jpg
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