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外胚层发育蛋白通过 NF-κB 调节激素非依赖性乳腺导管形态发生。

Ectodysplasin regulates hormone-independent mammary ductal morphogenesis via NF-κB.

机构信息

Developmental Biology Program, Institute of Biotechnology, University of Helsinki, 00014 Helsinki, Finland.

出版信息

Proc Natl Acad Sci U S A. 2012 Apr 10;109(15):5744-9. doi: 10.1073/pnas.1110627109. Epub 2012 Mar 26.

Abstract

Ductal growth of the mammary gland occurs in two distinct stages. The first round of branching morphogenesis occurs during embryogenesis, and the second round commences at the onset of puberty. Currently, relatively little is known about the genetic networks that control the initial phases of ductal expansion, which, unlike pubertal development, proceeds independent of hormonal input in female mice. Here we identify NF-κB downstream of the TNF-like ligand ectodysplasin (Eda) as a unique regulator of embryonic and prepubertal ductal morphogenesis. Loss of Eda, or inhibition of NF-κB, led to smaller ductal trees with fewer branches. On the other hand, overexpression of Eda caused a dramatic NF-κB-dependent phenotype in both female and male mice characterized by precocious and highly increased ductal growth and branching that correlated with enhanced cell proliferation. We have identified several putative transcriptional target genes of Eda/NF-κB, including PTHrP, Wnt10a, and Wnt10b, as well as Egf family ligands amphiregulin and epigen. We developed a mammary bud culture system that allowed us to manipulate mammary development ex vivo and found that recombinant PTHrP, Wnt3A, and Egf family ligands stimulate embryonic branching morphogenesis, suggesting that these pathways may cooperatively mediate the effects of Eda.

摘要

乳腺导管的生长发生在两个不同的阶段。第一轮分支形态发生发生在胚胎发生期间,第二轮在青春期开始时开始。目前,相对较少的遗传网络控制着导管扩张的初始阶段,这与青春期发育不同,在雌性小鼠中,导管扩张独立于激素输入。在这里,我们确定 TNF 样配体外胚层发育素(Eda)下游的 NF-κB 是胚胎期和青春期前导管形态发生的独特调节剂。Eda 的缺失或 NF-κB 的抑制导致导管树更小,分支更少。另一方面,Eda 的过表达导致雌性和雄性小鼠中出现戏剧性的 NF-κB 依赖性表型,其特征是导管生长和分支的早熟和高度增加,与增强的细胞增殖相关。我们已经鉴定了几个 Eda/NF-κB 的潜在转录靶基因,包括 PTHrP、Wnt10a 和 Wnt10b 以及 Egf 家族配体 Amphiregulin 和 Epigen。我们开发了一种乳腺芽培养系统,使我们能够在体外操纵乳腺发育,并发现重组 PTHrP、Wnt3A 和 Egf 家族配体刺激胚胎分支形态发生,这表明这些途径可能协同介导 Eda 的作用。

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