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Rspo 1通过Wnt信号通路促进成骨细胞分化。

Rspo 1 promotes osteoblast differentiation via Wnt signaling pathway.

作者信息

Sharma Ashish R, Choi Byung-Soo, Park Jong-Min, Lee Dong-Hyun, Lee Jeong-Eun, Kim Hae-Sung, Yoon Jeong-Kyo, Song Dong-Keun, Nam Ju-Suk, Lee Sang-Soo

机构信息

Institute for Skeletal Aging & Orthopedic Surgery, Hallym University-Chuncheon Sacred Heart Hospital, Chucheon 200704, Korea.

出版信息

Indian J Biochem Biophys. 2013 Feb;50(1):19-25.

Abstract

R-spondin (Rspo)s proteins are a new group of Wnt/beta-catenin signaling agonists. These signaling molecules are known to be involved in the developmental stages of skeletal system. Recent studies in various murine osteoblast models have proposed that Rspo 1 may interact with Wnt signaling pathway to induce differentiation in osteoblasts. Though findings in murine osteoblasts implicate a synergestic role of Rspo 1 with Wnt signaling, still no study has addressed the similar role in more clinically applicable osteoblast models i.e., human cell lines or primary cells. Therefore, in the present study, we investigated the possible role of Rspo 1 during differentiation process of human in vitro osteoblast cell models like primary osteoblasts or human osteoprogenitor cell line hFOB 1.19 along with murine preosteoblast cell line MC3T3 E-1. Our results showed increase in Rspo 1 at transcript level during differentiating phase of human primary osteoblasts and human FOB 1.19 cells. We also found that Rspo 1 (100 ng/mL) acts additively with Wnt3a to activate Wnt signaling, as confirmed by luciferase activity after transfection of TOPFLASH construct to hFOB 1.19 cells. Similar additive role of Rspo 1 and Wnt3a was apparent in alkaline phosphatase (ALP) activity analysis of human primary cells. Moreover, a reduction in ALP activity was observed with knock-down of Rspo 1 by transfected shRNA in hFOB 1.19 cells. These results suggested the possibility of autocrine regulation by Rspo 1 on the osteogenic activities in human in vitro osteoblast models. Furthermore, these results were corroborated in MC3T3-E1, murine osteoblast cell model. Osteoblastic differentiation was induced by transfection of Rspo 1 which was confirmed by increased ALP staining and qRT-PCR analysis of osteogenic markers, such as Runx2 and osteocalcin. In conclusion, present study highlights the role of Rspo 1 in bone remodeling where it activates Wnt signaling to induce differentiation, as shown in human as well murine in vitro osteoblast cell models.

摘要

R-spondin(Rspo)蛋白是一组新的Wnt/β-连环蛋白信号激动剂。已知这些信号分子参与骨骼系统的发育阶段。最近在各种小鼠成骨细胞模型中的研究表明,Rspo 1可能与Wnt信号通路相互作用以诱导成骨细胞分化。尽管在小鼠成骨细胞中的研究结果表明Rspo 1与Wnt信号具有协同作用,但仍没有研究探讨其在更具临床适用性的成骨细胞模型(即人类细胞系或原代细胞)中的类似作用。因此,在本研究中,我们研究了Rspo 1在人类体外成骨细胞模型(如原代成骨细胞或人类骨祖细胞系hFOB 1.19)以及小鼠前成骨细胞系MC3T3 E-1的分化过程中可能发挥的作用。我们的结果显示,在人类原代成骨细胞和人类FOB 1.19细胞的分化阶段,Rspo 1的转录水平升高。我们还发现,Rspo 1(100 ng/mL)与Wnt3a具有相加作用以激活Wnt信号,这在将TOPFLASH构建体转染至hFOB 1.19细胞后通过荧光素酶活性得到证实。在人类原代细胞的碱性磷酸酶(ALP)活性分析中,Rspo 1和Wnt3a的类似相加作用也很明显。此外,在hFOB 1.19细胞中,通过转染shRNA敲低Rspo 1后观察到ALP活性降低。这些结果表明,在人类体外成骨细胞模型中,Rspo 1对成骨活性存在自分泌调节的可能性。此外,这些结果在小鼠成骨细胞模型MC3T3-E1中得到了证实。通过转染Rspo 1诱导成骨细胞分化,这通过增加的ALP染色以及对成骨标志物(如Runx2和骨钙素)的qRT-PCR分析得到证实。总之,本研究强调了Rspo 1在骨重塑中的作用,即在人类和小鼠体外成骨细胞模型中,它激活Wnt信号以诱导分化。

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