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Lhx2是一种直接的NF-κB靶基因,可促进初级毛囊基板向下生长。

Lhx2 is a direct NF-κB target gene that promotes primary hair follicle placode down-growth.

作者信息

Tomann Philip, Paus Ralf, Millar Sarah E, Scheidereit Claus, Schmidt-Ullrich Ruth

机构信息

Department of Signal Transduction in Tumor Cells, Max-Delbrück-Center (MDC) for Molecular Medicine, Berlin 13092, Germany.

Department of Dermatology, University of Münster, Münster 48149, Germany Dermatological Science Research Group, Centre for Dermatology Research, Institute of Inflammation and Repair, University of Manchester, Manchester M13 9PL, UK.

出版信息

Development. 2016 May 1;143(9):1512-22. doi: 10.1242/dev.130898. Epub 2016 Mar 7.

Abstract

In the epidermis of mice lacking transcription factor nuclear factor-kappa B (NF-κB) activity, primary hair follicle (HF) pre-placode formation is initiated without progression to proper placodes. NF-κB modulates WNT and SHH signaling at early stages of HF development, but this does not fully account for the phenotypes observed upon NF-κB inhibition. To identify additional NF-κB target genes, we developed a novel method to isolate and transcriptionally profile primary HF placodes with active NF-κB signaling. In parallel, we compared gene expression at the same developmental stage in NF-κB-deficient embryos and controls. This uncovered novel NF-κB target genes with potential roles in priming HF placodes for down-growth. Importantly, we identify Lhx2 (encoding a LIM/homeobox transcription factor) as a direct NF-κB target gene, loss of which replicates a subset of phenotypes seen in NF-κB-deficient embryos. Lhx2 and Tgfb2 knockout embryos exhibit very similar abnormalities in HF development, including failure of the E-cadherin suppression required for follicle down-growth. We show that TGFβ2 signaling is impaired in NF-κB-deficient and Lhx2 knockout embryos and that exogenous TGFβ2 rescues the HF phenotypes in Lhx2 knockout skin explants, indicating that it operates downstream of LHX2. These findings identify a novel NF-κB/LHX2/TGFβ2 signaling axis that is crucial for primary HF morphogenesis, which may also function more broadly in development and disease.

摘要

在缺乏转录因子核因子-κB(NF-κB)活性的小鼠表皮中,初级毛囊(HF)前基板形成开始,但无法进展为正常基板。NF-κB在HF发育早期调节WNT和SHH信号通路,但这并不能完全解释NF-κB抑制后观察到的表型。为了鉴定额外的NF-κB靶基因,我们开发了一种新方法来分离具有活跃NF-κB信号的初级HF基板并对其进行转录谱分析。同时,我们比较了NF-κB缺陷胚胎和对照在相同发育阶段的基因表达。这揭示了在启动HF基板向下生长中具有潜在作用的新的NF-κB靶基因。重要的是,我们鉴定Lhx2(编码一种LIM/同源框转录因子)为直接的NF-κB靶基因,其缺失复制了NF-κB缺陷胚胎中观察到的一部分表型。Lhx2和Tgfb2基因敲除胚胎在HF发育中表现出非常相似的异常,包括毛囊向下生长所需的E-钙黏蛋白抑制失败。我们表明,TGFβ2信号通路在NF-κB缺陷和Lhx2基因敲除胚胎中受损,并且外源性TGFβ2可挽救Lhx2基因敲除皮肤外植体中的HF表型,表明它在LHX2下游起作用。这些发现确定了一个新的NF-κB/LHX2/TGFβ2信号轴,该信号轴对初级HF形态发生至关重要,其在发育和疾病中可能也具有更广泛的作用。

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