Auto and transactivation of FGF expression: potential mechanism for regulation of myogenic differentiation.

J C Fox, J L Swain
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引用次数: 8

Abstract

Fibroblast growth factors (FGFs) are potent inhibitors of myogenic differentiation. The recent observation that the endogenous expression of acidic and basic FGF by myogenic cells decreases coordinately with differentiation suggests a regulatory role for these growth factors in myogenesis. Inasmuch as other proteins known to influence myogenesis (e.g., MyoD1 and myogenin) activate their own expression as well as the expression of other members of their family, we hypothesized that the FGFs might be capable of similar autoregulation. We examined the effect of exogenously supplied FGF on the abundance of the mRNAs encoding acidic and basic FGF in Sol 8 myoblasts, and demonstrate that either acidic or basic FGF stimulate, through paracrine mechanisms, the accumulation of the mRNAs encoding both of these FGFs. Thus FGFs can auto- and transregulate their own expression in a manner analogous to that observed for the myogenic determination proteins. In addition, similar to that previously observed for MyoD1, both acidic and basic FGF suppress myogenin expression in myoblasts. These results suggest two mechanisms whereby endogenously produced FGFs participate in the maintenance of the undifferentiated state of myogenic cells. These data provide support for paracrine, and suggest potential autocrine, roles for FGFs in the regulation of myogenic differentiation.

FGF表达的自动和反激活:调节肌源性分化的潜在机制。
成纤维细胞生长因子(FGFs)是肌源性分化的有效抑制剂。最近观察到,内源性的酸性和碱性FGF在肌生成细胞中的表达随着分化而减少,这表明这些生长因子在肌生成中起调节作用。由于已知影响肌肉发生的其他蛋白质(例如MyoD1和myogenin)激活其自身及其家族其他成员的表达,我们假设FGFs可能具有类似的自我调节能力。我们研究了外源性FGF对Sol 8成肌细胞中酸性和碱性FGF编码mrna丰度的影响,并证明酸性或碱性FGF通过旁分泌机制刺激编码这两种FGF的mrna的积累。因此,FGFs可以以类似于观察到的肌原性决定蛋白的方式自动调节和反调节其自身的表达。此外,与先前观察到的MyoD1相似,酸性和碱性FGF都抑制成肌细胞中肌原素的表达。这些结果提示了两种机制,即内源性产生的FGFs参与维持肌原细胞的未分化状态。这些数据支持旁分泌,并提示潜在的自分泌,FGFs在调节肌源性分化中的作用。
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