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核糖体中密码子-反密码子相互作用的机制。tRNA与大肠杆菌30-S核糖体亚基的密码子依赖性结合的定量研究。

The mechanism of codon-anticodon interaction in ribosomes. Quantitative study of codon-dependent binding of tRNA to the 30-S ribosomal subunits of Escherichia coli.

作者信息

Kirillov S V, Makhno V I, Semenkov Y P

出版信息

Eur J Biochem. 1978 Aug 15;89(1):297-304. doi: 10.1111/j.1432-1033.1978.tb20927.x.

Abstract

The formation of a ternary complex 30-S-subunit . poly(U) . tRNAPhe is discussed and the conditions for its correct description by Langmuir's isotherm are deduced. The affinity constant of the binary complex 30-S-subunit . poly(U) is measured. The reversibility of binding of tRNAPhe to the complex 30-S-subunit . poly(U) is proved in a direct way. The main reason for the heterogeneity of ternary complexes was found to be due to the ability of high-molecular-weight poly(U) to form complicated aggregates with 30-S subunits. If a fraction of poly(U) of moderate molecular weight (30 000) is used, then the ternary complexes are homogeneous in stability and yield the same affinity constants for deacylated, aminoacylated and peptidyl-tRNAPhe (1 X 10(8) M-1 at 20 mM Mg2+, 200 mM NH+4 and 0 degrees C). Ribosomal protein S1 increases the binding constant of poly(U) with 30-S subunits but does not change the binding constant of tRNAPhe with the 30-S-subunit . poly(U) complex. All 30-S subunits, even partially stripped of S1 protein, are active in the binding of both poly(U) and tRNAPhe.

摘要

讨论了三元复合物30-S亚基·聚(U)·苯丙氨酰-tRNAphe的形成,并推导了用朗缪尔等温线对其进行正确描述的条件。测量了二元复合物30-S亚基·聚(U)的亲和常数。直接证明了苯丙氨酰-tRNAphe与复合物30-S亚基·聚(U)结合的可逆性。发现三元复合物异质性的主要原因是高分子量聚(U)能够与30-S亚基形成复杂的聚集体。如果使用一部分中等分子量(30000)的聚(U),那么三元复合物在稳定性上是均匀的,并且对于脱酰基、氨酰基和肽基-苯丙氨酰-tRNAphe产生相同的亲和常数(在20 mM Mg2+、200 mM NH4+和0℃下为1×108 M-1)。核糖体蛋白S1增加了聚(U)与30-S亚基的结合常数,但不改变苯丙氨酰-tRNAphe与30-S亚基·聚(U)复合物的结合常数。所有30-S亚基,即使部分去除了S1蛋白,在聚(U)和苯丙氨酰-tRNAphe的结合中都具有活性。

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