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小鼠肾脏中的鸟氨酸脱羧酶信使核糖核酸:一种由雄激素调控、具有快速动力学的低丰度基因产物。

Ornithine decarboxylase mRNA in mouse kidney: a low abundancy gene product regulated by androgens with rapid kinetics.

作者信息

Jänne O A, Kontula K K, Isomaa V V, Bardin C W

出版信息

Ann N Y Acad Sci. 1984;438:72-84. doi: 10.1111/j.1749-6632.1984.tb38277.x.

Abstract

We have used ODC gene expression in mouse kidney as the biological marker for studies of early androgen action. Some of the characteristics of this regulation involve its strict androgen specificity, the dependency on functional androgen receptors, the lack of requirement for pituitary hormones, and the ability of physiological androgens to bring about activation of the ODC gene. Some recent findings have revealed an additional intriguing feature in the regulation of ODC gene expression in that androgen sensitivity of ODC stimulation is genetically regulated in the mouse kidney (unpublished observations). One of the mechanisms by which androgens regulate renal ODC synthesis is to increase the concentration of ODC mRNA. Increased accumulation of this mRNA was seen as soon as 6 hr after testosterone administration, and it peaked 24 hr posttreatment. In general, acute changes in immunoreactive ODC concentration and ODC mRNA accumulation had very similar kinetics, suggesting that androgens induced de novo synthesis of ODC by increasing the rate of ODC gene transcription. In addition, there was always a highly significant correlation between the catalytic enzyme activity and immunoreactive enzyme protein concentration indicating that androgens do not specifically regulate the active site of ODC by either activating or inhibiting the enzyme by posttranslational modifications. A typical feature of ODC in virtually all eukaryotic tissues is the extremely rapid turnover rate of the enzyme with a biological half-life of 10-30 min. However, no direct information on the turnover rate of ODC mRNA is currently available, although indirect experiments have assigned a half-life of about seven hours for this mRNA. The availability of cDNA clones for ODC mRNA measurements will now permit us to address this question more directly, and also to investigate a possible role of androgens in the stabilization of ODC mRNA. In this regard it is of interest to note that chronic treatment of mice with pharmacological doses of testosterone prolongs the half-life of ODC protein four- to tenfold.

摘要

我们已将小鼠肾脏中的鸟氨酸脱羧酶(ODC)基因表达用作早期雄激素作用研究的生物学标志物。这种调节的一些特征包括其严格的雄激素特异性、对功能性雄激素受体的依赖性、对垂体激素的无需性,以及生理性雄激素激活ODC基因的能力。最近的一些发现揭示了ODC基因表达调节中另一个有趣的特征,即小鼠肾脏中ODC刺激的雄激素敏感性受基因调控(未发表的观察结果)。雄激素调节肾脏ODC合成的机制之一是增加ODC mRNA的浓度。睾酮给药后6小时即可观察到这种mRNA的积累增加,并在治疗后24小时达到峰值。一般来说,免疫反应性ODC浓度和ODC mRNA积累的急性变化具有非常相似的动力学,表明雄激素通过增加ODC基因转录速率诱导ODC的从头合成。此外,催化酶活性与免疫反应性酶蛋白浓度之间始终存在高度显著的相关性,表明雄激素不会通过翻译后修饰激活或抑制酶来特异性调节ODC的活性位点。几乎所有真核组织中ODC的一个典型特征是该酶的周转速度极快,生物学半衰期为10 - 30分钟。然而,目前尚无关于ODC mRNA周转速度的直接信息,尽管间接实验已确定该mRNA的半衰期约为7小时。用于ODC mRNA测量的cDNA克隆的可用性现在将使我们能够更直接地解决这个问题,并研究雄激素在ODC mRNA稳定中的可能作用。在这方面,值得注意的是,用药理剂量的睾酮对小鼠进行长期治疗可使ODC蛋白的半衰期延长4至10倍。

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