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生长激素诱导的骨基因表达的全基因组微阵列分析:新型转录因子T-box3调节成骨细胞增殖。

Whole genome microarray analysis of growth hormone-induced gene expression in bone: T-box3, a novel transcription factor, regulates osteoblast proliferation.

作者信息

Govoni Kristen E, Lee Seong Keun, Chadwick Robert B, Yu Hongrun, Kasukawa Yuji, Baylink David J, Mohan Subburaman

机构信息

Musculoskeletal Disease Center (151 Jerry L. Pettis Memorial Veterans Affairs Medical Center, 11201 Benton St., Loma Linda, CA 92357, USA.

出版信息

Am J Physiol Endocrinol Metab. 2006 Jul;291(1):E128-36. doi: 10.1152/ajpendo.00592.2005. Epub 2006 Feb 7.

Abstract

Growth hormone (GH) is important in the development and maintenance of bone; however, the IGF-dependent and -independent molecular pathways involved remain to be established. We used microarray analysis to evaluate GH signaling pathways in 4-wk-old GH-deficient mice following a single injection of GH (4 mg/kg body wt) or PBS (n = 6/group) at 6 or 24 h after treatment. Six thousand one hundred sixty genes were differentially expressed at P </= 0.05, and 17% of these genes were identified at both time points. Several of the genes differentially expressed were expressed sequence tags, and the remaining genes fell into 49 Gene Ontology categories. For subsequent studies, we focused on T-box (Tbx)3, a novel transcription factor, which increased more than twofold at both time points. Real-time RT-PCR analysis determined that pretreatment with IGF-binding protein-4 did not block GH-induced Tbx3 expression in vitro. Pretreatment with TNF-alpha blocked GH-induced Tbx3 expression. Tbx3 expression increased during osteoblast differentiation and following BMP-7 and Wnt3a treatment (P </= 0.05). Blocking Tbx3 expression by small interfering RNA decreased cell number and [(3)H]Thymidine incorporation (P < 0.01). In conclusion, 1) GH caused acute changes in several novel genes, suggesting that many GH-induced signaling pathways and target genes remain to be discovered; 2) because Tbx3 expression is regulated in osteoblasts and blockage of Tbx3 expression decreased cell number and DNA synthesis, we propose that Tbx3 is an important determinant of osteoblast cell number.

摘要

生长激素(GH)在骨骼的发育和维持中起着重要作用;然而,所涉及的依赖胰岛素样生长因子(IGF)和不依赖IGF的分子途径仍有待确定。我们使用微阵列分析来评估4周龄GH缺乏小鼠在单次注射GH(4mg/kg体重)或PBS(每组n = 6)后6小时或24小时的GH信号通路。在P≤0.05时,有6160个基因差异表达,其中17%的基因在两个时间点均被鉴定出来。差异表达的基因中有几个是表达序列标签,其余基因分为49个基因本体类别。在后续研究中,我们重点关注了一种新型转录因子T盒(Tbx)3,其在两个时间点均增加了两倍以上。实时逆转录聚合酶链反应(RT-PCR)分析确定,用IGF结合蛋白-4预处理并不能在体外阻断GH诱导的Tbx3表达。用肿瘤坏死因子-α(TNF-α)预处理可阻断GH诱导的Tbx3表达。在成骨细胞分化过程中以及在骨形态发生蛋白-7(BMP-7)和Wnt3a处理后,Tbx3表达增加(P≤0.05)。用小干扰RNA阻断Tbx3表达可减少细胞数量和[³H]胸腺嘧啶掺入量(P < 0.01)。总之,1)GH导致了几个新基因的急性变化,这表明许多GH诱导的信号通路和靶基因仍有待发现;2)由于Tbx3表达在成骨细胞中受到调控,且阻断Tbx3表达会减少细胞数量和DNA合成,我们提出Tbx3是成骨细胞数量的一个重要决定因素。

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