RAM结构域和锚蛋白重复序列在成骨细胞系细胞中对Notch信号传导及活性的作用。

Role of the RAM domain and ankyrin repeats on notch signaling and activity in cells of osteoblastic lineage.

作者信息

Deregowski Valerie, Gazzerro Elisabetta, Priest Leah, Rydziel Sheila, Canalis Ernesto

机构信息

Department of Research Saint Francis Hospital and Medical Center, Hartford, Connecticut 06105-1299, USA.

出版信息

J Bone Miner Res. 2006 Aug;21(8):1317-26. doi: 10.1359/jbmr.060505.

DOI:10.1359/jbmr.060505

PMID:16869730

Abstract

UNLABELLED

Notch proteins belong to a family of single pass transmembrane receptors that are activated after interactions with the membrane-bound ligands Delta and Jagged/Serrate. We determined the pathways responsible for the inhibitory effects of Notch on osteoblastogenesis and the contributions of the RAM domain and ankyrin repeats to this process in cells of the osteoblastic lineage.

INTRODUCTION

Notch receptors play a role in osteoblast differentiation. Activation of Notch results in its cleavage and the release of its intracellular domain (NICD), which interacts with the CBF1/RBP-Jkappa, Suppressor of Hairless, Lag-1 (CSL) family of transcription factors. The interaction is presumably mediated by the RBP-Jkappa-associated module (RAM) of NICD, although the role of the ankyrin repeats is uncertain.

MATERIALS AND METHODS

To determine the contributions of the RAM domain and ankyrin repeats to the inhibitory effects of Notch on osteoblastogenesis, ST-2 and MC3T3-E1 cells were transfected or transduced with vectors expressing NICD, RAM (NICD DeltaRAM), and ankyrin (NICD DeltaANK) deletion mutants.

RESULTS

Notch increased the transactivation of transiently transfected 12xCSL-Luc constructs, containing 12 repeats of an RBP-Jkappa/CSL binding site, and of the hairy and E (spl) (HES)-1 promoter. Deletion of the ankyrin repeats resulted in the loss of 12xCSL-Luc and HES-1 promoter transactivation, whereas deletion of the RAM domain caused a partial loss of 12xCSL-Luc and sustained HES-1 promoter transactivation. NICD overexpression inhibited osteocalcin mRNA levels and alkaline phosphatase activity in ST-2 cells, and deletion of the ankyrin repeats, and to a lesser extent of the RAM domain, resulted in loss of the NICD inhibitory effect. NICD inhibited Wnt signaling and deletion of ankyrin repeats or the RAM domain restored Wnt signaling activity.

CONCLUSIONS

The RAM domain and ankyrin repeats are required for Notch signaling and activity, and the CSL pathway is central to the inhibitory effect of Notch on osteoblastogenesis.

摘要

未标记

Notch蛋白属于单次跨膜受体家族，在与膜结合配体Delta和Jagged/Serrate相互作用后被激活。我们确定了Notch对成骨细胞生成产生抑制作用的相关途径，以及RAM结构域和锚蛋白重复序列在成骨细胞谱系细胞这一过程中的作用。

引言

Notch受体在成骨细胞分化中发挥作用。Notch的激活导致其裂解并释放细胞内结构域（NICD），该结构域与CBF1/RBP-Jκ、无毛抑制因子、Lag-1（CSL）转录因子家族相互作用。这种相互作用可能是由NICD的RBP-Jκ相关模块（RAM）介导的，尽管锚蛋白重复序列的作用尚不确定。

材料与方法

为了确定RAM结构域和锚蛋白重复序列对Notch抑制成骨细胞生成作用的贡献，用表达NICD、RAM（NICDΔRAM）和锚蛋白（NICDΔANK）缺失突变体的载体转染或转导ST-2和MC3T3-E1细胞。

结果

Notch增加了瞬时转染的含12个RBP-Jκ/CSL结合位点重复序列的12xCSL-Luc构建体以及毛状和E（spl）（HES）-1启动子的反式激活。锚蛋白重复序列的缺失导致12xCSL-Luc和HES-1启动子反式激活丧失，而RAM结构域的缺失导致12xCSL-Luc部分丧失反式激活且HES-1启动子持续反式激活。NICD过表达抑制ST-2细胞中骨钙素mRNA水平和碱性磷酸酶活性，锚蛋白重复序列的缺失以及程度较轻的RAM结构域的缺失导致NICD抑制作用丧失。NICD抑制Wnt信号通路，锚蛋白重复序列或RAM结构域的缺失恢复Wnt信号通路活性。