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RBP-J 在 Notch 信号通路中扮演着两种相互对立的角色。

Two opposing roles of RBP-J in Notch signaling.

机构信息

Research Institute, Shiga Medical Center, Moriyama, Shiga, Japan.

出版信息

Curr Top Dev Biol. 2010;92:231-52. doi: 10.1016/S0070-2153(10)92007-3.

DOI:10.1016/S0070-2153(10)92007-3
PMID:20816397
Abstract

RBP-J/Su(H)/Lag1, the main transcriptional mediator of Notch signaling, binds DNA with the consensus sequence YRTGDGAD. Notch target genes can be controlled by two opposing activities of RBP-J. The interaction of the Notch intracellular domain with RBP-J induces a weak transcriptional activation and requires an additional tissue-specific transcriptional activator such as bHLH proteins or GATA to mediate strong target gene expression. For example, during Drosophila sensory organ precursor (SOP) cell development, proneural bHLH interacts with Da, a Drosophila orthologue of E2A, to form a tissue-specific activator of Su(H), the Drosophila orthologue of RBP-J. This complex and Su(H) act synergistically to promote the epidermal cell fate. In contrast, a complex of Su(H) with Hairless, a Drosophila functional homologue of MINT, has transcriptional repression activity that promotes SOP differentiation to neurons. Recent conditional loss-of-function studies demonstrated that transcriptional networks involving RBP-J, MINT, and E2A are conserved in mammalian cell differentiation, including multiple steps of lymphocyte development, and probably also in neuronal maturation in adult neurogenesis. During neurogenesis, Notch-RBP-J signaling was thought historically to be involved mainly in the maintenance of undifferentiated neural progenitors. However, the identification of a tissue-specific transcriptional activator of RBP-J-Notch has revealed new roles of RBP-J in the promotion of neuronal maturation. Finally, the Notch-independent function of RBP-J was recently discovered and will be reviewed here.

摘要

RBP-J/Su(H)/Lag1 是 Notch 信号转导的主要转录中介物,与 YRTGDGAD 共识序列结合 DNA。Notch 靶基因可以通过 RBP-J 的两种相反活性来控制。Notch 细胞内结构域与 RBP-J 的相互作用诱导弱转录激活,并需要额外的组织特异性转录激活剂,如 bHLH 蛋白或 GATA,以介导强靶基因表达。例如,在果蝇感觉器官前体细胞(SOP)细胞发育过程中,神经前 bHLH 与 Da(果蝇 E2A 的同源物)相互作用,形成 Su(H)的组织特异性激活物,果蝇 RBP-J 的同源物。该复合物和 Su(H)协同作用促进表皮细胞命运。相比之下,Su(H)与 Hairless 的复合物具有转录抑制活性,促进 SOP 分化为神经元。最近的条件性基因缺失研究表明,涉及 RBP-J、MINT 和 E2A 的转录网络在哺乳动物细胞分化中是保守的,包括淋巴细胞发育的多个步骤,并且可能在成年神经发生中的神经元成熟中也是如此。在神经发生过程中,历史上认为 Notch-RBP-J 信号主要参与未分化神经祖细胞的维持。然而,RBP-J 的组织特异性转录激活剂的鉴定揭示了 RBP-J 在促进神经元成熟中的新作用。最后,最近发现了 Notch 非依赖性的 RBP-J 功能,本文将对此进行综述。

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