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构巢曲霉中的胞外阿拉伯糖苷酶:不同cre突变对酶水平的影响。

Extracellular arabinases in Aspergillus nidulans: the effect of different cre mutations on enzyme levels.

作者信息

van der Veen P, Arst H N, Flipphi M J, Visser J

机构信息

Section Molecular Genetics of Industrial Microorganisms, Wageningen Agricultural University, The Netherlands.

出版信息

Arch Microbiol. 1994;162(6):433-40. doi: 10.1007/BF00282109.

Abstract

The regulation of the syntheses of two arabinan-degrading extracellular enzymes and several intracellular L-arabinose catabolic enzymes was examined in wild-type and carbon catabolite derepressed mutants of Aspergillus nidulans. alpha-L-Arabinofuranosidase B, endoarabinase, L-arabinose reductase, L-arabitol dehydrogenase, xylitol dehydrogenase, and L-xylulose reductase were all inducible to varying degrees by L-arabinose and L-arabitol and subject to carbon catabolite repression by D-glucose. With the exception of L-xylulose reductase, all were clearly under the control of creA, a negative-acting wide domain regulatory gene mediating carbon catabolite repression. Measurements of intracellular enzyme activities and of intracellular concentrations of arabitol and xylitol in mycelia grown on D-glucose in the presence of inducer indicated that carbon catabolite repression diminishes, but does not prevent uptake of inducer. Mutations in creA resulted in an apparently, in some instances very marked, elevated inducibility, perhaps reflecting an element of "self" catabolite repression by the inducing substrate. creA mutations also resulted in carbon catabolite derepression to varying degrees. The regulatory effects of a mutation in creB and in creC, two genes whose roles are unclear, but likely to be indirect, were, when observable, more modest. As with previous data showing the effect of creA mutations on structural gene expression, there were striking instances of phenotypic variation amongst creA mutant alleles and this variation followed no discernible pattern, i.e. it was non-hierarchical. This further supports molecular data obtained elsewhere, indicating a direct role for creA in regulating structural gene expression, and extends the range of activities under creA control.

摘要

在构巢曲霉的野生型和碳分解代谢物阻遏解除突变体中,研究了两种阿拉伯聚糖降解胞外酶和几种胞内L-阿拉伯糖分解代谢酶的合成调控。α-L-阿拉伯呋喃糖苷酶B、内切阿拉伯聚糖酶、L-阿拉伯糖还原酶、L-阿拉伯糖醇脱氢酶、木糖醇脱氢酶和L-木酮糖还原酶均在不同程度上被L-阿拉伯糖和L-阿拉伯糖醇诱导,并受到D-葡萄糖的碳分解代谢物阻遏。除L-木酮糖还原酶外,所有这些酶显然都受creA的控制,creA是一个介导碳分解代谢物阻遏的负作用宽域调控基因。在诱导剂存在下于D-葡萄糖上生长的菌丝体中,对胞内酶活性以及阿拉伯糖醇和木糖醇的胞内浓度进行测量,结果表明碳分解代谢物阻遏会减弱,但不会阻止诱导剂的摄取。creA中的突变导致诱导性明显升高,在某些情况下非常显著,这可能反映了诱导底物的“自身”分解代谢物阻遏作用。creA突变还导致不同程度的碳分解代谢物阻遏解除。creB和creC这两个基因的作用尚不清楚,但可能是间接的,其突变的调控效应(若可观察到)则较为适度。正如先前显示creA突变对结构基因表达影响的数据一样,creA突变等位基因之间存在显著的表型变异实例,且这种变异没有可辨别的模式,即是非等级性的。这进一步支持了在其他地方获得的分子数据,表明creA在调节结构基因表达方面具有直接作用,并扩展了受creA控制的活性范围。

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