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金黄色葡萄球菌中乳糖和D-半乳糖降解的D-塔格糖6-磷酸途径生理意义的遗传学证据。

Genetic evidence for the physiological significance of the D-tagatose 6-phosphate pathway of lactose and D-galactose degradation in staphylococcus aureus.

作者信息

Bissett D L, Anderson R L

出版信息

J Bacteriol. 1974 Sep;119(3):698-704. doi: 10.1128/jb.119.3.698-704.1974.

Abstract

Mutants of Staphylococcus aureus were isolated which were unable to utilize d-galactose or lactose, but which were able to utilize all other carbohydrates tested. Growth of the mutants on a peptone-containing medium was inhibited by d-galactose. Of those mutants selected for further study, one (tagI2) was missing d-galactose 6-phosphate isomerase, one (tagK3) was missing d-tagatose 6-phosphate kinase, and one (tagA4) was missing d-tagatose 1, 6-diphosphate aldolase. Each of these mutants accumulated the substrate of the missing enzyme intracellularly. Spontaneous revertants of each of the mutants simultaneously regained their ability to utilize d-galactose and lactose, lost their sensitivity to d-galactose, regained the missing enzymatic activities, and no longer accumulated intermediates of the d-tagatose 6-phosphate pathway. These data support our previous contention that the physiologically significant route for the metabolism of d-galactose and the d-galactosyl moiety of lactose in S. aureus is the d-tagatose 6-phosphate pathway. Furthermore, a mutant constitutive for all three enzymes of this pathway was isolated, indicating that the products of the tagI, tagK, and tagA genes are under common genetic control. This conclusion was supported by the demonstration that d-galactose 6-phosphate isomerase, d-tagatose 6-phosphate kinase, and d-tagatose 1, 6-diphosphate aldolase are coordinately induced in the parental strain.

摘要

分离出了金黄色葡萄球菌的突变体,这些突变体无法利用D-半乳糖或乳糖,但能够利用所测试的所有其他碳水化合物。在含蛋白胨的培养基上,突变体的生长受到D-半乳糖的抑制。在那些被选作进一步研究的突变体中,一个(tagI2)缺失D-半乳糖6-磷酸异构酶,一个(tagK3)缺失D-塔格糖6-磷酸激酶,一个(tagA4)缺失D-塔格糖1,6-二磷酸醛缩酶。这些突变体中的每一个都在细胞内积累了缺失酶的底物。每个突变体的自发回复突变体同时恢复了利用D-半乳糖和乳糖的能力,失去了对D-半乳糖的敏感性,恢复了缺失的酶活性,并且不再积累D-塔格糖6-磷酸途径的中间产物。这些数据支持了我们之前的观点,即金黄色葡萄球菌中D-半乳糖和乳糖的D-半乳糖基部分代谢的生理重要途径是D-塔格糖6-磷酸途径。此外,分离出了该途径所有三种酶的组成型突变体,这表明tagI、tagK和tagA基因的产物受到共同的遗传控制。D-半乳糖6-磷酸异构酶、D-塔格糖6-磷酸激酶和D-塔格糖1,6-二磷酸醛缩酶在亲本菌株中被协同诱导,这一证明支持了这一结论。

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