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星形孢菌素对绒毛膜癌细胞中人血清素转运体的非环磷酸腺苷依赖性上调作用。

Cyclic AMP-independent up-regulation of the human serotonin transporter by staurosporine in choriocarcinoma cells.

作者信息

Ramamoorthy J D, Ramamoorthy S, Papapetropoulos A, Catravas J D, Leibach F H, Ganapathy V

机构信息

Department of Biochemistry and Molecular Biology, Medical College of Georgia, Augusta 30912, USA.

出版信息

J Biol Chem. 1995 Jul 21;270(29):17189-95. doi: 10.1074/jbc.270.29.17189.

Abstract

Treatment of confluent cultures of JAR human placental choriocarcinoma cells with staurosporine caused a marked stimulation of serotonin transport activity in these cells. The stimulatory effect was noticeable at nanomolar concentrations of staurosporine, and a treatment time of > 4 h was required for staurosporine to elicit the effect. At 40 nM and with a treatment time of 16 h, the stimulation of the transport activity was 3.5-6.0-fold. None of the several other protein kinase inhibitors tested had similar effect except KT 5720, a protein kinase A inhibitor, which showed a small but significant (approximately 1.4-fold) stimulatory effect at a concentration of 5 microM. Blockade of RNA synthesis and protein synthesis in the cells prevented completely the stimulation of the transport activity induced by staurosporine. The stimulation was observed not only in intact cells but also in plasma membrane vesicles prepared from staurosporine-treated cells. The stimulation was accompanied by a 5-7-fold increase in the steady state levels of the transporter-specific mRNAs, by a 7-fold increase in the maximal velocity of the transport process, and by a 6-fold increase in the transporter density in the plasma membrane. Even though both staurosporine and cholera toxin had similar effects on the serotonin transport activity in these cells, the effect was not additive when the cells were treated with both reagents together. While treatment of the cells with cholera toxin markedly elevated intracellular levels of cAMP, staurosporine did not have any effect on the cellular levels of this cyclic nucleotide. It is concluded that staurosporine up-regulates the serotonin transport activity in JAR cells by increasing the steady state levels of the serotonin transporter mRNA and by the consequent increase in the transporter density in the plasma membrane and that the process involves a cAMP-independent signaling pathway.

摘要

用星形孢菌素处理JAR人胎盘绒毛膜癌细胞的汇合培养物,可显著刺激这些细胞中的5-羟色胺转运活性。在纳摩尔浓度的星形孢菌素下即可观察到刺激作用,且星形孢菌素引发该效应需要>4小时的处理时间。在40 nM且处理时间为16小时时,转运活性的刺激倍数为3.5至6.0倍。除蛋白激酶A抑制剂KT 5720外,所测试的其他几种蛋白激酶抑制剂均无类似作用,KT 5720在5 microM浓度时显示出较小但显著的(约1.4倍)刺激作用。细胞中RNA合成和蛋白质合成的阻断完全阻止了星形孢菌素诱导的转运活性刺激。不仅在完整细胞中观察到了这种刺激,在从经星形孢菌素处理的细胞制备的质膜囊泡中也观察到了。这种刺激伴随着转运体特异性mRNA稳态水平增加5至7倍、转运过程最大速度增加7倍以及质膜中转运体密度增加6倍。尽管星形孢菌素和霍乱毒素对这些细胞中的5-羟色胺转运活性有类似作用,但当细胞同时用这两种试剂处理时,该作用并无叠加效应。虽然用霍乱毒素处理细胞可显著提高细胞内cAMP水平,但星形孢菌素对这种环核苷酸的细胞水平没有任何影响。结论是,星形孢菌素通过增加5-羟色胺转运体mRNA的稳态水平以及随之而来的质膜中转运体密度增加,上调JAR细胞中的5-羟色胺转运活性,且该过程涉及一条不依赖cAMP的信号通路。

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