粗糙脉孢菌精氨酸途径中通量的控制。酶活性和浓度的调节。
Control of the flux in the arginine pathway of Neurospora crassa. Modulations of enzyme activity and concentration.
作者信息
Flint H J, Tateson R W, Barthelmess I B, Porteous D J, Donachie W D, Kacser H
出版信息
Biochem J. 1981 Nov 15;200(2):231-46. doi: 10.1042/bj2000231.
The influence of particular enzyme activities on the flux of metabolites in a pathway can be estimated by 'modulating' enzymes (i.e. changing turnover or concentration) and measuring the response in various parts of the system. By controlling the nuclear ration of two genetically different nuclear types in heterokaryons, the enzyme concentrations at four different steps in the arginine pathway were decreased over a range. This range was extended by the use of bradytrophs, mutant strains specifying enzymes with greatly diminished enzyme activities. Strains altered simultaneously at more than one step were also constructed by genetic recombination. By measuring the outputs of the pathway and the steady-state concentrations of intermediate pools, the fluxes in different parts of the pathway were calculated. This allowed the construction of flux/enzyme relationships, the slope of which is a measure of the sensitivity of a flux to the change in enzyme activity at that step. All fluxes were found to be considerably buffered for quite substantial decreases in the activities of all enzymes. Mass action plays an important part in this phenomenon, as do inhibition and repression. Because of the existence of expansion fluxes in growing systems, we find quantitatively different fluxes in different parts of the single pathway. For the same reason some enzyme modulations given decreased fluxes in one part and increased fluxes in another. The understanding of control in the pathway thus involves consideration of many mechanisms operating simultaneously and the estimation of changes in the whole system. The concept of a 'rate-limiting step' is found to be inadequate and is replaced by a quantitative measure, the Sensitivity Coefficient, which takes account of all the interactions. It is shown that control of the flux is shared among all the enzymes of the pathway. The results are discussed in terms of the theory of flux control.
特定酶活性对代谢途径中代谢物通量的影响可通过“调节”酶(即改变周转率或浓度)并测量系统各部分的响应来估算。通过控制异核体中两种遗传上不同核型的核比例,精氨酸途径中四个不同步骤的酶浓度在一定范围内降低。通过使用缓殖体(即指定酶活性大大降低的酶的突变菌株),这个范围得以扩大。还通过基因重组构建了在多个步骤同时发生改变的菌株。通过测量途径的输出和中间池的稳态浓度,计算出途径不同部分的通量。这使得能够构建通量/酶关系,其斜率衡量了通量对该步骤酶活性变化的敏感性。结果发现,对于所有酶活性相当大幅度的降低,所有通量都有相当程度的缓冲。质量作用在这一现象中起着重要作用,抑制和阻遏也是如此。由于生长系统中存在扩展通量,我们发现在单个途径的不同部分通量在数量上有所不同。出于同样的原因,一些酶调节在一部分中使通量降低,而在另一部分中使通量增加。因此,对途径中控制的理解涉及对许多同时起作用机制的考虑以及对整个系统变化的估计。发现“限速步骤”的概念并不充分,取而代之的是一种定量测量方法——敏感性系数,它考虑了所有的相互作用。结果表明,通量的控制由途径中的所有酶共同分担。根据通量控制理论对结果进行了讨论。
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