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发育中大脑的蛋白质降解速率。方法学考量。

The rate of protein degradation in developing brain. Methodological considerations.

作者信息

Dunlop D S, McHale D M, Lajtha A

出版信息

Biochem J. 1982 Dec 15;208(3):659-66. doi: 10.1042/bj2080659.

Abstract

Recently we reported that the rate of protein breakdown decreases during development. Breakdown rates were calculated from the rates of protein synthesis and the changes in brain protein content with age. A different study, measuring breakdown by monitoring the loss of label from brain protein after an H14CO3- pulse, came to the opposite conclusion: that the rate of breakdown is low in immature brain and increases during development. We have now investigated some of the factors (the distribution of label in protein and the potential for recycling) that might introduce errors into these measurements. The specific radioactivities of both protein-bound and free amino acids were determined in the brains of young rats several days after an intraperitoneal pulse of H14CO3-. For a number of amino acids the specific radioactivity of the free amino acid is high compared with that of the protein-bound amino acid, and therefore recycling could result in an underestimate of the degradation rate. Because glutamic acid had a relatively low specific-radioactivity ratio, [1-14C]glutamic acid was used in a pulse-labelling experiment to measure degradation. The rate so obtained, 0.6% . h-1, is twice the rate found with H14CO3- labelling (based on total protein-bound radioactivity). Insofar as recycling is a possible complication, 0.6% . h-1 may be a minimum value. Although somewhat higher degradation rates are found after labelling with an intracranial pulse, which was considered as a possible route to limit recycling, there are difficulties in interpreting these data.

摘要

最近我们报道,在发育过程中蛋白质分解速率下降。分解速率是根据蛋白质合成速率以及脑蛋白质含量随年龄的变化来计算的。另一项研究通过监测H14CO3-脉冲后脑蛋白质中标记物的损失来测量分解,却得出了相反的结论:即未成熟脑的分解速率较低,且在发育过程中增加。我们现在研究了一些可能会给这些测量带来误差的因素(蛋白质中标记物的分布以及再循环的可能性)。在腹腔注射H14CO3-几天后,测定了幼鼠脑中蛋白质结合型和游离氨基酸的比放射性。对于多种氨基酸而言,游离氨基酸的比放射性高于蛋白质结合型氨基酸,因此再循环可能导致对降解速率的低估。由于谷氨酸的比放射性相对较低,所以在脉冲标记实验中使用[1-14C]谷氨酸来测量降解。由此获得的速率为0.6%·h-1,是用H14CO3-标记法(基于蛋白质结合的总放射性)所发现速率的两倍。就再循环可能是一个复杂因素而言,0.6%·h-1可能是一个最小值。尽管在用颅内脉冲标记后发现了稍高的降解速率(颅内脉冲被认为是限制再循环的一种可能途径),但在解释这些数据时存在困难。

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Measurement of protein turnover in rat brain.大鼠大脑中蛋白质周转率的测量。
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