Effect of Translation-Enhancing Nascent SKIK Peptide on the Arrest Peptides Containing Consecutive Proline.

IF 3.7 2区 生物学 Q1 BIOCHEMICAL RESEARCH METHODS ACS Synthetic Biology Pub Date : 2024-11-21 DOI:10.1021/acssynbio.4c00221
Yuma Nishikawa, Riko Fujikawa, Hideo Nakano, Takashi Kanamori, Teruyo Ojima-Kato
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Abstract

Ribosome arrest peptides (RAPs) such as the SecM arrest peptide (SecM AP: FSTPVWISQAQGIRAGP) and WPPP with consecutive Pro residues are known to induce translational stalling in Escherichia coli. We demonstrate that the translation-enhancing SKIK peptide tag, which consists of four amino acid residues Ser-Lys-Ile-Lys, effectively alleviates translational arrest caused by WPPP. Moreover, the proximity between SKIK and WPPP significantly influences the extent of this alleviation, observed in both PURE cell-free protein synthesis and in vivo protein production systems, resulting in a substantial increase in the yield of proteins containing such RAPs. Furthermore, we unveil that nascent SKIK peptide tag and translation elongation factor P (EF-P) alleviate ribosome stalling in consecutive-Pro-rich protein to synergistically promote translation. A kinetic analysis based on the generation of superfolder green fluorescent protein under in vitro translation reaction reveals that the ribosome turnover is enhanced by more than 10-fold when the SKIK peptide tag is positioned immediately upstream of the SecM AP sequence. Our findings provide valuable insights into optimizing protein production processes, which are essential for advancing synthetic biology applications.

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翻译增强型新生 SKIK 肽对含有连续脯氨酸的停滞肽的影响
众所周知,核糖体停滞肽(RAPs),如 SecM 停滞肽(SecM AP:FSTPVWISQAQGIRAGP)和带有连续 Pro 残基的 WPPP 会诱导大肠杆菌的翻译停滞。我们证明,由 Ser-Lys-Ile-Lys 四个氨基酸残基组成的翻译增强 SKIK 肽标记能有效缓解 WPPP 引起的翻译停滞。此外,SKIK 和 WPPP 之间的接近程度会显著影响这种缓解的程度,这是在纯化无细胞蛋白质合成和体内蛋白质生产系统中观察到的,结果是含有这种 RAP 的蛋白质产量大幅增加。此外,我们还揭示了新生 SKIK 肽标记和翻译伸长因子 P(EF-P)可减轻富含连续蛋白的核糖体停滞,从而协同促进翻译。基于体外翻译反应下生成的超级绿色荧光蛋白的动力学分析表明,当 SKIK 肽标记紧靠 SecM AP 序列上游时,核糖体的周转率提高了 10 倍以上。我们的研究结果为优化蛋白质生产过程提供了宝贵的见解,这对推进合成生物学应用至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
8.00
自引率
10.60%
发文量
380
审稿时长
6-12 weeks
期刊介绍: The journal is particularly interested in studies on the design and synthesis of new genetic circuits and gene products; computational methods in the design of systems; and integrative applied approaches to understanding disease and metabolism. Topics may include, but are not limited to: Design and optimization of genetic systems Genetic circuit design and their principles for their organization into programs Computational methods to aid the design of genetic systems Experimental methods to quantify genetic parts, circuits, and metabolic fluxes Genetic parts libraries: their creation, analysis, and ontological representation Protein engineering including computational design Metabolic engineering and cellular manufacturing, including biomass conversion Natural product access, engineering, and production Creative and innovative applications of cellular programming Medical applications, tissue engineering, and the programming of therapeutic cells Minimal cell design and construction Genomics and genome replacement strategies Viral engineering Automated and robotic assembly platforms for synthetic biology DNA synthesis methodologies Metagenomics and synthetic metagenomic analysis Bioinformatics applied to gene discovery, chemoinformatics, and pathway construction Gene optimization Methods for genome-scale measurements of transcription and metabolomics Systems biology and methods to integrate multiple data sources in vitro and cell-free synthetic biology and molecular programming Nucleic acid engineering.
期刊最新文献
Advancements in Microbial Cell Engineering for Benzylisoquinoline Alkaloid Production. Structure-Guided Engineering Unveils Deeper Substrate Channel in Processive Endoglucanase EG5C-1 Contributing to Enhanced Catalytic Efficiency and Processivity. Carbon Negative Synthesis of Amino Acids Using a Cell-Free-Based Biocatalyst. Synthetic Ecosystems: From the Test Tube to the Biosphere. Effect of Translation-Enhancing Nascent SKIK Peptide on the Arrest Peptides Containing Consecutive Proline.
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