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首页> 外文期刊>Journal of bacteriology >Role of transport systems in amino acid metabolism: leucine toxicity and the branched-chain amino acid transport systems.
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Role of transport systems in amino acid metabolism: leucine toxicity and the branched-chain amino acid transport systems.

机译:转运系统在氨基酸代谢中的作用:亮氨酸毒性和支链氨基酸转运系统。

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摘要

The livR locus, which leads to a trans-recessive derepression of branched-chain amino acid transport and periplasmic branched-chain amino acid-binding proteins, is responsible for greatly increased sensitivity toward growth inhibition by leucine, valine, and serine and, as shown previously, for increased sensitivity toward toxicity by branched-chain amino acid analogues, such as 4-azaleucine or 5',5',5'-trifluoroleucine. These phenotypes are similar to those of relA mutants; however, the livR mutants retain the stringent response of ribonucleic acid synthesis. However, an increase in the rate of transport or in the steady-state intracellular level of amino acids in the livR strain cannot completely account for this sensitivity. The ability of the LIV-I transport system to carry out exchange of pool amino acids for extracellular leucine is a major factor in leucine sensitivity. The previous finding that inhibition of threonine deaminase by leucine contributes to growth inhibition is confirmed by simulating the in vivo conditions using a toluene-treated cell preparation with added amino acids at levels corresponding to the internal pool. The relationship between transport systems and corresponding biosynthetic pathways is discussed and the general principle of a coordination in the regulation of transport and biosynthetic pathways is forwarded. The finding that the LIV-I transport system functions well for amino acid exchange in contrast to the LIV-II system provides another feature that distinguishes these systems in addition to previously described differences in regulation and energetics.
机译:livR基因座导致分支链氨基酸转运和周质分支链氨基酸结合蛋白的反式隐性抑制,导致亮氨酸,缬氨酸和丝氨酸对生长抑制的敏感性大大提高,如图所示以前,为了提高支链氨基酸类似物对毒性的敏感性,例如4-氮杂亮氨酸或5',5',5'-三氟亮氨酸。这些表型与relA突变体的表型相似。然而,livR突变体保留了核糖核酸合成的严格反应。但是,livR菌株中氨基酸的转运速率或稳态细胞内氨基酸水平上的提高不能完全解释这种敏感性。 LIV-1转运系统进行池氨基酸交换为细胞外亮氨酸的能力是亮氨酸敏感性的主要因素。以前的发现,亮氨酸对苏氨酸脱氨酶的抑制有助于生长抑制,这是通过使用甲苯处理的细胞制备物模拟体内条件来证实的,该细胞制备物中添加了对应于内部库的氨基酸。讨论了运输系统和相应的生物合成途径之间的关系,并提出了协调运输和生物合成途径的一般原则。与LIV-II系统相反,LIV-I转运系统可很好地进行氨基酸交换的发现提供了另一个特征,除了先前描述的调节和能量学差异外,还可以区分这些系统。

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