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用tRNA底物类似物探测亮氨酰/苯丙氨酰tRNA蛋白质转移酶活性位点。

Probing the leucyl/phenylalanyl tRNA protein transferase active site with tRNA substrate analogues.

作者信息

Fung Angela Wai Shan, Ebhardt H Alexander, Krishnakumar Kollappillil S, Moore Jack, Xu Zhizhong, Strazewski Peter, Fahlman Richard P

机构信息

474 Medical Sciences Building. Department of Biochemistry. University of Alberta. Edmonton, Alberta, T6G 2H7, Canada.

出版信息

Protein Pept Lett. 2014 Jul;21(7):603-14. doi: 10.2174/0929866521666140212110639.

Abstract

Aminoacyl-tRNA protein transferases post-translationally conjugate an amino acid from an aminoacyl-tRNA onto the N-terminus of a target polypeptide. The eubacterial aminoacyl-tRNA protein transferase, L/F transferase, utilizes both leucyl-tRNA(Leu) and phenylalanyl-tRNA(Phe) as substrates. X-ray crystal structures with substrate analogues, the minimal substrate phenylalanyl adenosine (rA-Phe) and inhibitor puromycin, have been used to characterize tRNA recognition by L/F transferase. However analyses of these two X-ray crystal structures reveal significant differences in binding. Through structural analyses, mutagenesis, and enzymatic activity assays, we rationalize and demonstrate that the substrate analogues bind to L/F transferase with similar binding affinities using a series of different interactions by the various chemical groups of the analogues. Our data also demonstrates that enlarging the hydrophobic pocket of L/F transferase selectively enhances puromycin inhibition and may aid in the development of improved inhibitors for this class of enzymes.

摘要

氨酰基-tRNA蛋白转移酶在翻译后将氨酰基-tRNA上的氨基酸连接到目标多肽的N端。真细菌氨酰基-tRNA蛋白转移酶,即亮氨酸/苯丙氨酸转移酶,利用亮氨酰-tRNA(Leu)和苯丙氨酰-tRNA(Phe)作为底物。已使用与底物类似物、最小底物苯丙氨酰腺苷(rA-Phe)和抑制剂嘌呤霉素的X射线晶体结构来表征亮氨酸/苯丙氨酸转移酶对tRNA的识别。然而,对这两种X射线晶体结构的分析揭示了结合上的显著差异。通过结构分析、诱变和酶活性测定,我们进行了合理的分析并证明,底物类似物通过类似物的各种化学基团利用一系列不同的相互作用以相似的结合亲和力与亮氨酸/苯丙氨酸转移酶结合。我们的数据还表明,扩大亮氨酸/苯丙氨酸转移酶的疏水口袋可选择性增强嘌呤霉素抑制作用,并可能有助于开发针对这类酶的改进抑制剂。

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