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PTHrP and Skeletal Development

机译:PTHrP和骨骼发育

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摘要

Parathyroid hormone-related protein (PTHrP) participates in the regulation of endochondral bone development. After the cartilage mold is established in fetal life, perichondrial cells and chondro-cytes at the ends of the mold synthesize PTHrP. This ligand then acts on PTH/PTHrP receptors on chondrocytes. As chondrocytes go through a program of proliferation and then further differentiation into post-mitotic, hypertrophic chondrocytes, PTHrP action keeps chondrocytes proliferating and delays their further differentiation. Indian hedgehog (Ihh) is synthesized by chondrocytes that have just stopped proliferating and is required for synthesis of PTHrP. The feedback loop between PTHrP and Ihh serves to regulate the pace of chondrocyte differentiation and the sites at which perichondrial cells first differentiate into osteoblasts. Activation of the PTH/PTHrP receptor leads to stimulation of both G_s and G_q family heterotrimeric G proteins. Genetic analyses demonstrate that G_s activation mediates the action of PTHrP to keep chondrocytes proliferating, while G_q activation opposes this action. Downstream from G_s activation, synthesis of the cyclin-cdk inhibitor, p57, is suppressed, thereby increasing the pool of proliferating chondrocytes. PTHrP's actions to delay chondrocyte differentiation are mediated by the phosphorylation of the transcription factor, SOX9, and by suppression of synthesis of mRNA encoding the transcription factor, Runx2. These pathways and undoubtedly others cooperate to regulate the pace of differentiation of growth plate chondrocytes in response to PTHrP.
机译:甲状旁腺激素相关蛋白(PTHrP)参与软骨内骨发育的调节。在胎儿体内建立软骨霉菌后,霉菌末端的软骨膜细胞和软骨细胞合成了PTHrP。然后,该配体作用于软骨细胞上的PTH / PTHrP受体。当软骨细胞经历增殖程序,然后进一步分化为有丝分裂后的肥大性软骨细胞时,PTHrP的作用使软骨细胞增殖并延缓其进一步分化。印度刺猬(Ihh)由刚停止增殖的软骨细胞合成,是合成PTHrP所必需的。 PTHrP和Ihh之间的反馈回路用于调节软骨细胞分化的速度以及软骨膜细胞首次分化为成骨细胞的位置。 PTH / PTHrP受体的激活导致G_s和G_q家族异三聚体G蛋白的刺激。遗传分析表明,G_s激活介导了PTHrP的作用,以保持软骨细胞增殖,而G_q激活则反对该作用。在G_s激活的下游,细胞周期蛋白-cdk抑制剂p57的合成受到抑制,从而增加了增殖的软骨细胞库。 PTHrP延迟软骨细胞分化的作用是通过转录因子SOX9的磷酸化和抑制编码转录因子Runx2的mRNA合成来介导的。这些途径和毫无疑问的其他途径合作调节生长板软骨细胞对PTHrP的分化速度。

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