时钟基因影响小鼠生长板和软骨内骨化中的基因表达。

Clock genes influence gene expression in growth plate and endochondral ossification in mice.

机构信息

Laboratory of Molecular Pharmacology, Division of Pharmaceutical Sciences, Kanazawa University Graduate School, Kanazawa, Ishikawa 920-1192, Japan.

出版信息

J Biol Chem. 2012 Oct 19;287(43):36081-95. doi: 10.1074/jbc.M112.408963. Epub 2012 Aug 30.

Abstract

We have previously shown transient promotion by parathyroid hormone of Period-1 (Per1) expression in cultured chondrocytes. Here we show the modulation by clock genes of chondrogenic differentiation through gene transactivation of the master regulator of chondrogenesis Indian hedgehog (IHH) in chondrocytes of the growth plate. Several clock genes were expressed with oscillatory rhythmicity in cultured chondrocytes and rib growth plate in mice, whereas chondrogenesis was markedly inhibited in stable transfectants of Per1 in chondrocytic ATDC5 cells and in rib growth plate chondrocytes from mice deficient of brain and muscle aryl hydrocarbon receptor nuclear translocator-like (BMAL1). Ihh promoter activity was regulated by different clock gene products, with clear circadian rhythmicity in expression profiles of Ihh in the growth plate. In BMAL1-null mice, a predominant decrease was seen in Ihh expression in the growth plate with a smaller body size than in wild-type mice. BMAL1 deficit led to disruption of the rhythmic expression profiles of both Per1 and Ihh in the growth plate. A clear rhythmicity was seen with Ihh expression in ATDC5 cells exposed to dexamethasone. In young mice defective of BMAL1 exclusively in chondrocytes, similar abnormalities were found in bone growth and Ihh expression. These results suggest that endochondral ossification is under the regulation of particular clock gene products expressed in chondrocytes during postnatal skeletogenesis through a mechanism relevant to the rhythmic Ihh expression.

摘要

我们之前曾证明甲状旁腺激素(PTH)可短暂促进培养软骨细胞中 Period-1(Per1)的表达。在此,我们通过时钟基因对主调控因子印度刺猬因子(IHH)的基因转录激活,研究了时钟基因对软骨分化的调节作用,而主调控因子 IHH 在生长板中的软骨细胞中表达。在培养的软骨细胞和小鼠的长骨生长板中,有几个时钟基因表现出振荡节律性的表达,而在 Per1 稳定转染的 ATDC5 细胞和缺乏脑和肌肉芳香烃受体核转位蛋白样(BMAL1)的小鼠长骨生长板软骨细胞中,软骨发生明显受到抑制。Ihh 启动子活性受不同的时钟基因产物调节,在生长板中 Ihh 的表达具有明显的昼夜节律性。在 BMAL1 基因敲除的小鼠中,与野生型小鼠相比,其生长板中 Ihh 的表达明显减少,导致其体型较小。BMAL1 缺乏会导致生长板中 Per1 和 Ihh 的表达节律性紊乱。在 ATDC5 细胞中,DEX 可使 Ihh 的表达呈现出明显的节律性。在软骨细胞中特异性缺乏 BMAL1 的幼龄小鼠中,骨生长和 Ihh 表达也存在类似的异常。这些结果表明,软骨细胞中特定时钟基因产物的表达对软骨内成骨有调控作用,其调控机制与 IHH 表达的节律性有关。

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