A new bacterial tRNA enhances antibiotic production in Streptomyces by circumventing inefficient wobble base-pairing

Author:

Chen Ximing12,Li Shuyan3,Zhang Binglin24,Sun Haili5,Wang Jinxiu12,Zhang Wei12,Meng Wenbo6,Chen Tuo24,Dyson Paul7ORCID,Liu Guangxiu12

Affiliation:

1. Key Laboratory of Desert and Desertification, Northwest Institute of Eco-Environment and Resources , Chinese Academy of Sciences, Lanzhou , Gansu , China

2. Key Laboratory of Extreme Environmental Microbial Resources and Engineering , Lanzhou , Gansu , China

3. School of Medical Information and Engineering, Xuzhou Medical University , Jiangsu , China

4. State Key Laboratory of Cryospheric Sciences, Northwest Institute of Eco-Environment and Resources, Chinese Academy of Sciences , Lanzhou , Gansu , China

5. School of Chemistry and Environmental Science, Lanzhou City University , Lanzhou , Gansu , China

6. Key Laboratory of Biological Therapy and Regenerative Medicine Transformation Gansu Province; The First Clinical Medical School of Lanzhou University , China

7. Institute of Life Science, Swansea University Medical School , Singleton Park, Swansea SA2 8PP, UK

Abstract

Abstract We report the discovery and functional characterization of a new bacterial tRNA species. The tRNA-Asp-AUC, from a fast-growing desert streptomycete, decodes GAU codons. In the absence of queuosine tRNA anticodon modification in streptomycetes, the new tRNA circumvents inefficient wobble base-pairing during translation. The tRNA, which is constitutively expressed, greatly enhances synthesis of 4 different antibiotics in the model mesophilic species Streptomyces coelicolor, including the product of a so-called cryptic pathway, and increases yields of medically-important antibiotics in other species. This can be rationalised due to increased expression of both pleiotropic and pathway-specific transcriptional activators of antibiotic biosynthesis whose genes generally possess one or more GAT codons; the frequency of this codon in these gene sets is significantly higher than the average for streptomycete genes. In addition, the tRNA enhances production of cobalamin, a precursor of S-adenosyl methionine, itself an essential cofactor for synthesis of many antibiotics. The results establish a new paradigm of inefficient wobble base-pairing involving GAU codons as an evolved strategy to regulate gene expression and, in particular, antibiotic biosynthesis. Circumventing this by expression of the new cognate tRNA offers a generic strategy to increase antibiotic yields and to expand the repertoire of much-needed new bioactive metabolites produced by these valuable bacteria.

Funder

West Light Foundation of the Chinese Academy of Sciences

National Key Research and Development Program of China

National Science Foundation of China

UK BBSRC China

Gansu Youth Science and Technology

Publisher

Oxford University Press (OUP)

Subject

Genetics

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