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Get Free AccessAbstract CrAss-like phages are a recently described family-level group of viruses that includes the most abundant virus in the human gut 1,2 . Genomes of all crAss-like phages encode a large virion-packaged protein 2,3 that contains a DFDxD sequence motif, which forms the catalytic site in cellular multisubunit RNA polymerases (RNAPs) 4 . Using Cellulophaga baltica crAss-like phage phi14:2 as a model system, we show that this protein is a novel DNA-dependent RNAP that is translocated into the host cell along with the phage DNA and transcribes early phage genes. We determined the crystal structure of this 2,180-residue enzyme in a self-inhibited, likely pre-virion-packaged state. This conformation is attained with the help of a Cleft-blocking domain that interacts with the active site motif and occupies the RNA-DNA hybrid binding grove. Structurally, phi14:2 RNAP is most similar to eukaryotic RNAPs involved in RNA interference 5,6 , although most of phi14:2 RNAP structure (nearly 1,600 residues) maps to a new region of protein folding space. Considering the structural similarity, we propose that eukaryal RNA interference polymerases take their origin in a phage, which parallels the emergence of the mitochondrial transcription apparatus 7 .
Arina V. Drobysheva, Sofia A. Panafidina, Matvey Kolesnik, Evgeny Klimuk, Leonid Minakhin, Maria Yakunina, Sergei Borukhov, Emelie Nilsson, Karin Holmfeldt, Natalya Yutin, Kira S. Makarova, Eugene V Koonin, Konstantin Severinov, P.G. Leiman, Maria L. Sokolova (2020). Structure and function of virion RNA polymerase of crAss-like phage. , DOI: https://doi.org/10.1101/2020.03.07.982082.
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Type
Preprint
Year
2020
Authors
15
Datasets
0
Total Files
0
Language
en
DOI
https://doi.org/10.1101/2020.03.07.982082
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