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构巢曲霉中嘌呤羟化酶翻译后激活所必需的hxB基因,受嘌呤利用和烟酸利用转录激活系统的独立控制。

The hxB gene, necessary for the post-translational activation of purine hydroxylases in Aspergillus nidulans, is independently controlled by the purine utilization and the nicotinate utilization transcriptional activating systems.

作者信息

Amrani L, Cecchetto G, Scazzocchio C, Glatigny A

机构信息

Institut de Génétique et Microbiologie, Orsay, France.

出版信息

Mol Microbiol. 1999 Feb;31(4):1065-73. doi: 10.1046/j.1365-2958.1999.01242.x.

Abstract

Molybdenum-containing enzymes of the hydroxylase class (such as xanthine dehydrogenase, aldehyde oxidase and nicotinate dehydrogenase) require a terminal sulphur atom attached to the molybdenum to hydroxylate their specific substrates. The transulphurylation reaction is carried out in Drosophila melanogaster by the product of the ma-I gene. In Aspergillus nidulans, the activity of the isofunctional and homologous HxB protein is needed in at least two different metabolic contexts, when the organism grows on purines and when it grows on nicotinate as nitrogen sources. We show here that the expression of the hxB gene is not constitutive. It is induced independently and additively by the inducers of the purine and of the nicotinate utilization pathways. Each of these induction pathways is affected independently by mutations in their cognate genes, uric acid induction by mutations in the UaY protein and nicotinate and 6-nicotinate induction by those in the hxnR/aplA complex. It is, in both metabolic contexts, exquisitely sensitive to nitrogen metabolite repression and highly dependent on the AreA GATA factor.

摘要

羟化酶类含钼酶(如黄嘌呤脱氢酶、醛氧化酶和烟酸脱氢酶)需要一个连接在钼上的末端硫原子来使其特定底物羟化。转硫反应在黑腹果蝇中由ma-I基因的产物进行。在构巢曲霉中,当生物体以嘌呤为氮源生长以及以烟酸为氮源生长时,至少在两种不同的代谢环境中需要同功能且同源的HxB蛋白的活性。我们在此表明,hxB基因的表达不是组成型的。它由嘌呤利用途径和烟酸利用途径的诱导剂独立且累加地诱导。这些诱导途径中的每一个都受到其同源基因突变的独立影响,尿酸诱导受UaY蛋白突变的影响,烟酸和6-烟酸诱导受hxnR/aplA复合体中突变的影响。在这两种代谢环境中,它对氮代谢物阻遏极为敏感,并且高度依赖于AreA GATA因子。

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