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甲状旁腺激素与佛波酯对大鼠骨肉瘤细胞中活化蛋白-1基因家族成员的刺激作用

Parathyroid hormone versus phorbol ester stimulation of activator protein-1 gene family members in rat osteosarcoma cells.

作者信息

Koe R C, Clohisy J C, Tyson D R, Pulumati M R, Cook T F, Partridge N C

机构信息

Department of Pharmacological and Physiological Science, St. Louis University Health Sciences Center, 1402 South Grand Boulevard, St. Louis, Missouri 63104, USA.

出版信息

Calcif Tissue Int. 1997 Jul;61(1):52-8. doi: 10.1007/s002239900294.

Abstract

We have previously shown that in the rat osteoblastic osteosarcoma cell line-UMR 106-01-PTH induces maximal collagenase mRNA levels at 4 hours. Since this response to PTH requires de novo protein synthesis, it may be mediated by the combined temporal expression of members of the activator protein-1 (AP-1) gene family. We have demonstrated that maximal mRNA levels of two of the members of this family, c-fos and c-jun, occur 30 min after stimulation by PTH. Phorbol myristate acetate (PMA) elicits a similar increase in c-fos and c-jun mRNAs, but is unable to stimulate transcription of collagenase in these cells. To investigate further the involvement of the AP-1 gene family, we examined PTH and PMA stimulation of jun-B, jun-D, fos B, and fra-1 mRNAs in UMR 106-01 cells. The mRNA for jun-D was abundant under control conditions and showed no variation in response to PTH (10(-8) M). The fos B transcripts were not detected under control conditions, whereas jun-B and fra-1 mRNAs were present at low basal levels. PTH caused an increase in fos B mRNA that reached a maximal 4- to 5-fold plateau between 45 and 60 min. An increase in jun-B mRNA in response to PTH was detectable at 30 min, but reached a maximal 6- to 7-fold increase at 2 hours. After PTH stimulation, the fra-1 transcript showed a 10- to 11-fold peak at 4 hours. PMA (2.6 x 10(-7) M) stimulated fos B mRNA to maximal abundance at 1 hour, similar to PTH. In contrast, PMA caused a maximal increase in jun-B mRNA at 30 min and fra-1 mRNA at 2 hours, which was earlier than the response to PTH. To determine whether an increase in jun-B at the same time as c-fos and c-jun would inhibit collagenase gene transcription, we cotransfected an expression vector for jun-B with a rat collagenase promoter-reporter gene construct. This resulted in a decrease in PTH-stimulation of promoter activity. Thus, it appears that the differential temporal stimulation of the AP-1 genes by PTH and PMA, particularly an increase in jun-B at the same time as c-fos and c-jun, explains the difference seen in their ability to induce transcription of collagenase.

摘要

我们之前已经表明,在大鼠成骨细胞性骨肉瘤细胞系UMR 106 - 01中,甲状旁腺激素(PTH)在4小时时可诱导胶原酶mRNA水平达到最大值。由于这种对PTH的反应需要从头合成蛋白质,它可能是由激活蛋白-1(AP-1)基因家族成员的联合时序表达介导的。我们已经证明,该家族的两个成员c-fos和c-jun的mRNA水平在PTH刺激后30分钟达到最大值。佛波酯(PMA)可引起c-fos和c-jun mRNA的类似增加,但不能刺激这些细胞中胶原酶的转录。为了进一步研究AP-1基因家族的参与情况,我们检测了PTH和PMA对UMR 106 - 01细胞中jun-B、jun-D、fos B和fra-1 mRNA的刺激作用。在对照条件下,jun-D的mRNA含量丰富,对PTH(10^(-8) M)无反应变化。在对照条件下未检测到fos B转录本,而jun-B和fra-1 mRNA以低基础水平存在。PTH导致fos B mRNA增加,在45至60分钟之间达到最大4至5倍的平台期。在30分钟时可检测到PTH诱导的jun-B mRNA增加,但在2小时时达到最大6至7倍的增加。PTH刺激后,fra-1转录本在4小时时显示出10至11倍的峰值。PMA(2.6×10^(-7) M)在1小时时刺激fos B mRNA达到最大丰度,与PTH相似。相比之下,PMA在30分钟时使jun-B mRNA达到最大增加,在2小时时使fra-1 mRNA达到最大增加,这比PTH的反应更早。为了确定与c-fos和c-jun同时增加jun-B是否会抑制胶原酶基因转录,我们将jun-B的表达载体与大鼠胶原酶启动子-报告基因构建体共转染。这导致PTH对启动子活性的刺激作用降低。因此,似乎PTH和PMA对AP-1基因的不同时序刺激,特别是与c-fos和c-jun同时增加jun-B,解释了它们在诱导胶原酶转录能力上的差异。

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