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Let-7b Regulates Myoblast Proliferation by Inhibiting IGF2BP3 Expression in Dwarf and Normal Chicken

机译:Let-7b通过抑制矮人和正常鸡的IGF2BP3表达来调节成肌细胞增殖。

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摘要

The sex-linked dwarf chicken is caused by the mutation of growth hormone receptor (GHR) gene and characterized by shorter shanks, lower body weight, smaller muscle fiber diameter and fewer muscle fiber number. However, the precise regulatory pathways that lead to the inhibition of skeletal muscle growth in dwarf chickens still remain unclear. Here we found a let-7b mediated pathway might play important role in the regulation of dwarf chicken skeletal muscle growth. Let-7b has higher expression in the skeletal muscle of dwarf chicken than in normal chicken, and the expression of insulin-like growth factor 2 mRNA binding protein 3 (IGF2BP3), which is a translational activator of IGF2, showed opposite expression trend to let-7b. In vitro cellular assays validated that let-7b directly inhibits IGF2BP3 expression through binding to its 3′UTR region, and the protein level but not mRNA level of IGF2 would be reduced in let-7b overexpressed chicken myoblast. Let-7b can inhibit cell proliferation and induce cell cycle arrest in chicken myoblast through let-7b-IGF2BP3-IGF2 signaling pathway. Additionally, let-7b can also regulate skeletal muscle growth through let-7b-GHR-GHR downstream genes pathway, but this pathway is non-existent in dwarf chicken because of the deletion mutation of GHR 3′UTR. Notably, as the loss binding site of GHR for let-7b, let-7b has enhanced its binding and inhibition on IGF2BP3 in dwarf myoblast, suggesting that the miRNA can balance its inhibiting effect through dynamic regulate its binding to target genes. Collectively, these results not only indicate that let-7b can inhibit skeletal muscle growth through let-7b-IGF2BP3-IGF2 signaling pathway, but also show that let-7b regulates myoblast proliferation by inhibiting IGF2BP3 expression in dwarf and normal chickens.
机译:与性相关的矮鸡是由生长激素受体(GHR)基因突变引起的,其特征是小腿短,体重低,肌纤维直径小和肌纤维数少。然而,导致矮鸡骨骼肌生长受到抑制的确切调控途径仍不清楚。在这里,我们发现let-7b介导的途径可能在矮鸡骨骼肌生长的调节中起重要作用。 Let-7b在矮鸡的骨骼肌中的表达高于正常鸡,而胰岛素样生长因子2 mRNA结合蛋白3(IGF2BP3)的表达是IGF2的翻译激活因子,其表达趋势与let-7b相反。 -7b。体外细胞试验证实,let-7b通过与其3'UTR区结合而直接抑制IGF2BP3的表达,而过表达let-7b的鸡成肌细胞中IGF2的蛋白水平将降低,而IGF2的mRNA水平将降低。 Let-7b可通过let-7b-IGF2BP3-IGF2信号通路抑制鸡成肌细胞的细胞增殖并诱导细胞周期停滞。此外,let-7b还可以通过let-7b-GHR-GHR下游基因途径调节骨骼肌的生长,但是由于GHR 3'UTR的缺失突变,矮小鸡中不存在该途径。值得注意的是,由于let-7b的GHR失去了结合位点,let-7b增强了对矮生成肌细胞中IGF2BP3的结合和抑制,这表明miRNA可通过动态调节其与靶基因的结合来平衡其抑制作用。总的来说,这些结果不仅表明let-7b可以通过let-7b-IGF2BP3-IGF2信号通路抑制骨骼肌生长,而且还表明let-7b通过抑制侏儒和正常鸡的IGF2BP3表达来调节成肌细胞增殖。

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