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大肠杆菌甲硫氨酰转运RNA合成酶的转运RNA与氨基酸激活位点之间的相互关系

Interrelation between transfer RNA and amino-acid-activating sites of methionyl transfer RNA synthetase from Escherichia coli.

作者信息

Jacques Y, Blanquet S

出版信息

Eur J Biochem. 1977 Oct 3;79(2):433-41. doi: 10.1111/j.1432-1033.1977.tb11825.x.

Abstract

Binding of tRNA(Met/f) to the monomeric trypsin-modified methionyl-tRNA synthetase turns off the methionine-dependent isotopic ATP--PPi exchange. In the case of the dimeric native methionyltRNA synthetase, one anticooperatively bound tRNA(Met/f) inhibits the exchange by only 50%. These behaviours of tRNA do not require the integrity of the 3'-terminal adenosine. Esterification by methionine of the 3' end of tRNA reinforces the affinity of tRNA(Met/f)for the enzymes. In the case of the native enzyme, due to this effect, a second binding mode for methionyl-tRNA may be demonstrated through the isotopic exchange. This additional binding of tRNA corresponds to the expression of the anticooperatively blocked tRNA binding site. Methionine reverses competitively the reinforcing effect of the esterified methionyl moiety on tRNA binding. It is concluded that after esterification of tRNA, the aminoacyl residue still binds the enzyme, probably within the methionine activating site. The latter behaviour may account for the observation that excess methionine accelerates the aminoacylation turnover rate of tRNA(Met/f).

摘要

tRNA(Met/f)与单体胰蛋白酶修饰的甲硫氨酰-tRNA合成酶的结合会关闭甲硫氨酸依赖性的同位素ATP-PPi交换。对于二聚体天然甲硫氨酰-tRNA合成酶,一个反协同结合的tRNA(Met/f)仅抑制50%的交换。tRNA的这些行为不需要3'-末端腺苷的完整性。甲硫氨酸对tRNA 3'末端的酯化增强了tRNA(Met/f)对酶的亲和力。对于天然酶,由于这种效应,可以通过同位素交换证明甲硫氨酰-tRNA的第二种结合模式。tRNA的这种额外结合对应于反协同阻断的tRNA结合位点的表达。甲硫氨酸竞争性地逆转酯化甲硫氨酰部分对tRNA结合的增强作用。得出的结论是,tRNA酯化后,氨酰基残基仍与酶结合,可能在甲硫氨酸活化位点内。后一种行为可能解释了过量甲硫氨酸加速tRNA(Met/f)氨酰化周转率的现象。

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Methionyl-tRNA synthetase from Escherichia coli. Inactivation and labeling by periodate-treated initiator tRNA.
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