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经典的Notch信号传导在表皮谱系中作为一种决定开关发挥作用。

Canonical notch signaling functions as a commitment switch in the epidermal lineage.

作者信息

Blanpain Cédric, Lowry William E, Pasolli H Amalia, Fuchs Elaine

机构信息

Howard Hughes Medical Institute, The Rockefeller University, New York, NY 10021, USA.

出版信息

Genes Dev. 2006 Nov 1;20(21):3022-35. doi: 10.1101/gad.1477606.

Abstract

Mammalian epidermis consists of a basal layer of proliferative progenitors that gives rise to multiple differentiating layers to provide a waterproof envelope covering the skin surface. To accomplish this, progenitor cells must detach from the basal layer, move upward, and execute a terminal differentiation program consisting of three distinct stages: spinous, granular layer, and stratum corneum. Notch signaling has been implicated in late stages of differentiation, but the commitment switch remains unknown. Here we show with loss and gain-of-function studies that active Notch intracellular domain (NICD) and its obligate canonical signaling partner RBP-J act at the basal/suprabasal juncture to induce spinous and down-regulate basal fate. Spinous layers are absent in RBP-J conditional null epidermis and expanded when Notch1 signaling is elevated transgenically in epidermis. We show that RBP-J is essential for mediating both spinous gene activation and basal gene repression. In contrast, the NICD/RBP-J target gene Hes1 is expressed in spinous layers and mediates spinous gene induction but not basal gene repression. These data uncover an early role for RBP-J and Notch in commitment of epidermal cells to terminally differentiate and reveal that spinous gene induction is mediated by a Hes1-dependent mechanism, while basal gene repression occurs independently of Hes1.

摘要

哺乳动物的表皮由增殖祖细胞的基底层组成,该基底层产生多个分化层,以形成覆盖皮肤表面的防水包膜。为实现这一功能,祖细胞必须从基底层脱离,向上移动,并执行一个由三个不同阶段组成的终末分化程序:棘层、颗粒层和角质层。Notch信号通路已被证明与分化后期有关,但细胞命运决定的转换机制仍不清楚。在这里,我们通过功能缺失和功能获得研究表明,活性Notch胞内结构域(NICD)及其必需的经典信号转导伴侣RBP-J在基底/基底上层交界处发挥作用,诱导棘层形成并下调基底细胞命运。在RBP-J条件性敲除的表皮中不存在棘层,而当Notch1信号通路在表皮中通过转基因方式增强时,棘层会扩展。我们表明,RBP-J对于介导棘层基因激活和基底基因抑制都是必不可少的。相比之下,NICD/RBP-J靶基因Hes1在棘层中表达,并介导棘层基因诱导,但不介导基底基因抑制。这些数据揭示了RBP-J和Notch在表皮细胞终末分化决定中的早期作用,并表明棘层基因诱导是由一种依赖Hes1的机制介导的,而基底基因抑制则独立于Hes1发生。

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