首页> 外文期刊>Molecular and Cellular Endocrinology >IGF-1 or insulin, and the TSH cyclic AMP cascade separately control dog and human thyroid cell growth and DNA synthesis, and complement each other in inducing mitogenesis.
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IGF-1 or insulin, and the TSH cyclic AMP cascade separately control dog and human thyroid cell growth and DNA synthesis, and complement each other in inducing mitogenesis.

机译:IGF-1或胰岛素以及TSH环状AMP级联分别控制狗和人甲状腺细胞的生长和DNA合成,并在诱导有丝分裂中相互补充。

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摘要

The regular doubling of cell mass, and therefore of cell protein content, is required for repetitive cell divisions. Preliminary observations have shown that in dog thyrocytes insulin induces protein accumulation but not DNA synthesis, while TSH does not increase protein accumulation but triggers DNA synthesis in the presence of insulin. We show here that EGF and phorbol myristate ester complement insulin action in the same way. HGF is the only factor activating both protein accumulation and DNA synthesis. The effects of insulin on protein accumulation and in permitting the TSH effect are reproduced by IGF-1 and are mediated, at least in part by the IGF-1 receptor. The concentration effect curves are similar for both effects. Similar results are obtained in human thyrocytes. They reflect true cell growth, as shown by increases in RNA content and cell size. Carbachol and fetal calf serum also stimulate protein synthesis and accumulation without triggering DNA synthesis, but they are not permissive for the mitogenic effects of TSH or of the general adenylate cyclase activator, forskolin. Moreover the mitogenic effect of TSH greatly decreased in cells deprived of insulin for 2 days although these cells remain hypertrophic. Hypertrophy may therefore be necessary for cell division, but it is not sufficient to permit it. Three different mechanisms can therefore be distinguished in the mitogenic action of TSH: (1) the increase of cell mass (hypertrophy) induced by insulin or IGF-1; (2) the permissive effect of insulin or IGF-1 on the mitogenic effect of TSH which may involve both the increase of cell mass and the induction of specific proteins such as cyclin D3 and (3) the mitogenic effect of the TSH cyclic AMP cascade proper.
机译:重复的细胞分裂需要细胞质量的规则加倍,因此细胞蛋白质含量也需要加倍。初步观察结果表明,在犬甲状腺细胞中,胰岛素诱导蛋白质积累,但不诱导DNA合成,而TSH在胰岛素存在下不增加蛋白质积累,但触发DNA合成。我们在这里显示EGF和豆蔻酸佛波醇酯以相同的方式补充胰岛素作用。 HGF是激活蛋白质积累和DNA合成的唯一因素。胰岛素对蛋白质蓄积和允许TSH作用的作用由IGF-1再现,并且至少部分地由IGF-1受体介导。两种效应的浓度效应曲线相似。在人甲状腺细胞中获得了相似的结果。它们反映了真实的细胞生长,如RNA含量和细胞大小的增加所表明。卡巴胆碱和胎牛血清也可刺激蛋白质合成和积累而不会触发DNA合成,但它们不允许TSH或一般腺苷酸环化酶激活剂forskolin的促有丝分裂作用。而且,在缺乏胰岛素2天的细胞中,TSH的促有丝分裂作用大大降低,尽管这些细胞仍然肥大。因此,肥大对于细胞分裂可能是必需的,但仅允许它是不够的。因此,在TSH的促有丝分裂作用中可以区分三种不同的机制:(1)胰岛素或IGF-1诱导的细胞量增加(肥大); (2)胰岛素或IGF-1对TSH的促有丝分裂作用的放任作用,这可能涉及细胞量的增加和特定蛋白如细胞周期蛋白D3的诱导,以及(3)TSH环状AMP级联的促有丝分裂作用正确。

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