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生长激素调节与c-fos血清反应元件相关的三元复合因子和血清反应因子。

Growth hormone regulates ternary complex factors and serum response factor associated with the c-fos serum response element.

作者信息

Liao J, Hodge C, Meyer D, Ho P S, Rosenspire K, Schwartz J

机构信息

Department of Physiology, University of Michigan Medical School, Ann Arbor, Michigan 48109-0622, USA.

出版信息

J Biol Chem. 1997 Oct 10;272(41):25951-8. doi: 10.1074/jbc.272.41.25951.

Abstract

For insight into the mechanisms of gene regulation by growth hormone (GH), the regulation of transcription factors associated with the serum response element (SRE) located upstream of c-fos was examined. The SRE can mediate induction of reporter expression in response to GH. For insight into the mechanism by which GH regulates transcription factors, regulation of SRE-associated proteins by GH was examined. In nuclear extracts from 3T3-F442A fibroblasts, several SRE-binding complexes were identified by electrophoretic mobility shift assay. GH treatment for 2-10 min transiently increased binding of two complexes; binding returned to control values within 30 min. The two GH-stimulated complexes were supershifted by antibodies against the serum response factor (SRF), indicating that they contained SRF or an antigenically related protein. One of the GH-stimulated complexes was supershifted by antibody against Elk-1, suggesting that it contains a ternary complex factor (TCF) such as Elk-1 in addition to SRF. Induction of binding by GH was lost when the SRF binding site in the SRE was mutated, and mutation of either the SRF or TCF binding site altered the pattern of protein binding to the SRE. Mutation of the SRF or TCF binding site in SRE-luciferase plasmids inhibited the ability of GH to stimulate reporter expression, supporting a role for both SRF and TCF in GH-induced transcription of c-fos via the SRE. The TCF family member Elk-1 is capable of mediating GH-stimulated transcription, since GH-stimulated reporter expression was mediated by the transcriptional activation domain of Elk-1. Consistent with this stimulation, GH rapidly and transiently stimulated the serine phosphorylation of Elk-1. The increase was evident within 10 min and subsided after 30 min. Taken together, these data indicate that SRF and TCF contribute to GH-promoted transcription of c-fos via the SRE and are consistent with GH-promoted phosphorylation of Elk-1 contributing to GH-promoted transcriptional activation via the SRE.

摘要

为深入了解生长激素(GH)对基因调控的机制,研究了与c-fos上游血清反应元件(SRE)相关的转录因子的调控。SRE可介导报告基因表达对GH的诱导。为深入了解GH调节转录因子的机制,研究了GH对SRE相关蛋白的调控。在3T3-F442A成纤维细胞的核提取物中,通过电泳迁移率变动分析鉴定了几种SRE结合复合物。用GH处理2 - 10分钟可短暂增加两种复合物的结合;30分钟内结合恢复到对照值。两种受GH刺激的复合物被抗血清反应因子(SRF)的抗体超迁移,表明它们含有SRF或抗原相关蛋白。其中一种受GH刺激的复合物被抗Elk-1抗体超迁移,提示除SRF外它还含有三元复合物因子(TCF)如Elk-1。当SRE中的SRF结合位点发生突变时,GH诱导的结合丧失,且SRF或TCF结合位点的突变改变了蛋白质与SRE的结合模式。SRE - 荧光素酶质粒中SRF或TCF结合位点的突变抑制了GH刺激报告基因表达的能力,支持SRF和TCF在GH通过SRE诱导c-fos转录中的作用。TCF家族成员Elk-1能够介导GH刺激的转录,因为GH刺激的报告基因表达是由Elk-1的转录激活域介导的。与这种刺激一致,GH迅速且短暂地刺激了Elk-1的丝氨酸磷酸化。这种增加在10分钟内明显,30分钟后消退。综上所述,这些数据表明SRF和TCF通过SRE促进GH介导的c-fos转录,并且与GH促进的Elk-1磷酸化通过SRE促进GH介导的转录激活一致。

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