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沙门氏菌中酪氨酸和苯丙氨酸生物合成的调控

Regulation of tyrosine and phenylalanine biosynthesis in Salmonella.

作者信息

Sprinson D B, Gollub E G, Hu R C, Liu K P

出版信息

Acta Microbiol Acad Sci Hung. 1976;23(2):167-70.

PMID:9783
Abstract

Several types of 4-fluorophenylalanine resistant mutants were isolated. In one type of mutant DAHP synthetase (tyr) and prephenate dehydrogenase were coordinately derepressed. The mutation was linked to aroF and tyrA and was cis- dominant by merodiploid analysis, thus confirming that it is an operator constitutive mutation (tyrOc). A second type of mutation showed highly elevated levels of tyrosine pathway enzymes which were not repressed by L-tyrosine. It was unlinked to tyrA and aroF, and was trans-recessive in merodiploids. These properties were attributed to a mutation in a regulator gene, tyrR (linked to pyr F), that resulted in altered or non-functional aporepressor. Hence tyrO, tyrA, and aroF constitute an operon regulated by tyrR. In a third type of mutation chorismate mutase P-prephenate dehydratase was highly elevated. It was not linked to pheA, was located in the 95--100 min region of the Salmonella chromosome, and was recessive to the wild type gene in merodiploids. A mutation was, therefore, indicated in a regulatory gene, pheR, which specified an aporepressor for regulating pheA. DAHP synthetase (phe), specified by aroG, was not regulated by pheR, but was derepressed in one of the tyrR mutants, suggesting that as in Escherichia coli tyrR may regulate DAHP synthetase(phe) and DAHP synthetase (tyr) with the same aporepressor. A novel mutation in chorismate mutase is described.

摘要

分离出了几种对4-氟苯丙氨酸具有抗性的突变体。在一种突变体中,DAHP合酶(tyr)和预苯酸脱氢酶协同去阻遏。该突变与aroF和tyrA连锁,通过部分二倍体分析呈顺式显性,从而证实它是一个操纵子组成型突变(tyrOc)。第二种突变类型显示酪氨酸途径酶的水平高度升高,且不受L-酪氨酸抑制。它与tyrA和aroF不连锁,在部分二倍体中呈反式隐性。这些特性归因于调节基因tyrR(与pyrF连锁)中的突变,该突变导致变构或无功能的脱辅阻遏物。因此,tyrO、tyrA和aroF构成一个由tyrR调控的操纵子。在第三种突变类型中,分支酸变位酶P-预苯酸脱水酶高度升高。它与pheA不连锁,位于沙门氏菌染色体的95-100分钟区域,在部分二倍体中对野生型基因呈隐性。因此,表明在一个调节基因pheR中发生了突变,该基因指定了一种用于调节pheA的脱辅阻遏物。由aroG指定的DAHP合酶(phe)不受pheR调控,但在一个tyrR突变体中去阻遏,这表明与大肠杆菌一样,tyrR可能用相同的脱辅阻遏物调节DAHP合酶(phe)和DAHP合酶(tyr)。描述了一种分支酸变位酶的新突变。

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