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胰岛素和胰岛素样生长因子I在神经突形成过程中对微管蛋白mRNA的稳定作用。

Stabilization of tubulin mRNAs by insulin and insulin-like growth factor I during neurite formation.

作者信息

Fernyhough P, Mill J F, Roberts J L, Ishii D N

机构信息

Department of Physiology, Colorado State University, Fort Collins 80523.

出版信息

Brain Res Mol Brain Res. 1989 Nov;6(2-3):109-20. doi: 10.1016/0169-328x(89)90044-2.

Abstract

Neurotrophic factors may increase axon and dendrite growth in part by regulating the content of cytoskeletal elements such as microtubules, which are comprised of tubulin subunits. The mechanism by which insulin, insulin-like growth factors (IGFs), and nerve growth factor (NGF) can increase the relative abundance of tubulin mRNAs as a prelude to neurite formation was studied. Insulin significantly increased the abundance of tubulin mRNAs relative to total RNA in cultured human neuroblastoma SH-SY5Y cells. This increase was not the result of a generalized elevation of all transcripts, because tubulin mRNAs were elevated relative to poly(A)+ RNA as well. Moreover, whereas polymerases I and III were elevated in activity, polymerase II was not. Tubulin mRNAs were stabilized against degradation in the presence of actinomycin D by both insulin and IGF-I. In contrast, actin and histone 3.3 mRNAs were neither increased nor stabilized. Insulin did not alter alpha- or beta-tubulin gene transcription rates in nuclear run-off experiments, and did increase the relative synthesis of tubulin proteins. These results suggest that tubulin mRNA levels are increased mainly through selective stabilization by insulin and IGFs. Because NGF is known to stabilize tubulin mRNA levels also, stabilization of tubulin mRNAs is suggested to be a common event in the pathway leading to neurite elongation directed by neuritogenic polypeptides.

摘要

神经营养因子可能部分通过调节细胞骨架成分(如由微管蛋白亚基组成的微管)的含量来促进轴突和树突的生长。研究了胰岛素、胰岛素样生长因子(IGF)和神经生长因子(NGF)作为神经突形成前奏增加微管蛋白mRNA相对丰度的机制。在培养的人神经母细胞瘤SH-SY5Y细胞中,胰岛素相对于总RNA显著增加了微管蛋白mRNA的丰度。这种增加并非所有转录本普遍升高的结果,因为相对于聚腺苷酸加尾RNA(poly(A)+ RNA),微管蛋白mRNA也有所升高。此外,虽然聚合酶I和III的活性升高,但聚合酶II没有。在放线菌素D存在的情况下,胰岛素和IGF-I都能稳定微管蛋白mRNA不被降解。相比之下,肌动蛋白和组蛋白3.3的mRNA既没有增加也没有被稳定。在核转录实验中,胰岛素没有改变α-或β-微管蛋白基因的转录速率,但确实增加了微管蛋白的相对合成。这些结果表明,微管蛋白mRNA水平主要通过胰岛素和IGF的选择性稳定而增加。由于已知NGF也能稳定微管蛋白mRNA水平,因此微管蛋白mRNA的稳定被认为是在神经生成多肽引导的神经突伸长途径中的一个常见事件。

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