A phage nucleus-associated RNA-binding protein is required for jumbo phage infection

Author:

Enustun Eray1,Armbruster Emily G1ORCID,Lee Jina1,Zhang Sitao2,Yee Brian A2,Malukhina Kseniya2,Gu Yajie2,Deep Amar2,Naritomi Jack T2,Liang Qishan2,Aigner Stefan2,Adler Benjamin A34ORCID,Cress Brady F4ORCID,Doudna Jennifer A3456789,Chaikeeratisak Vorrapon10,Cleveland Don W211,Ghassemian Majid12,Bintu Bogdan2,Yeo Gene W211,Pogliano Joe1,Corbett Kevin D1211ORCID

Affiliation:

1. Department of Molecular Biology, University of California San Diego , La Jolla , CA  92093 , USA

2. Department of Cellular and Molecular Medicine, University of California San Diego , La Jolla , CA  92093 , USA

3. California Institute for Quantitative Biosciences (QB3), University of California , Berkeley , CA  94720 , USA

4. Innovative Genomics Institute, University of California , Berkeley , CA  94720 , USA

5. Department of Molecular and Cell Biology, University of California , Berkeley , CA  94720 , USA

6. Department of Chemistry, University of California , Berkeley , CA  94720 , USA

7. Howard Hughes Medical Institute, University of California , Berkeley , CA  94720 , USA

8. Environmental Genomics and Systems Biology Division, Lawrence Berkeley National Laboratory , Berkeley , CA  94720 , USA

9. MBIB Division, Lawrence Berkeley National Laboratory , Berkeley , CA  94720 , USA

10. Department of Biochemistry, Faculty of Science, Chulalongkorn University , Bangkok  10330 , Thailand

11. Moores Cancer Center, University of California at San Diego , La Jolla , CA , USA

12. Biomolecular and Proteomics Mass Spectrometry Facility, University of California San Diego , La Jolla , CA  92093 , USA

Abstract

Abstract Large-genome bacteriophages (jumbo phages) of the proposed family Chimalliviridae assemble a nucleus-like compartment bounded by a protein shell that protects the replicating phage genome from host-encoded restriction enzymes and DNA-targeting CRISPR-Cas nucleases. While the nuclear shell provides broad protection against host nucleases, it necessitates transport of mRNA out of the nucleus-like compartment for translation by host ribosomes, and transport of specific proteins into the nucleus-like compartment to support DNA replication and mRNA transcription. Here, we identify a conserved phage nuclear shell-associated protein that we term Chimallin C (ChmC), which adopts a nucleic acid-binding fold, binds RNA with high affinity in vitro, and binds phage mRNAs in infected cells. ChmC also forms phase-separated condensates with RNA in vitro. Targeted knockdown of ChmC using mRNA-targeting dCas13d results in accumulation of phage-encoded mRNAs in the phage nucleus, reduces phage protein production, and compromises virion assembly. Taken together, our data show that the conserved ChmC protein plays crucial roles in the viral life cycle, potentially by facilitating phage mRNA translocation through the nuclear shell to promote protein production and virion development.

Funder

National Institutes of Health

Howard Hughes Medical Institute Emerging Pathogens Initiative

Howard Hughes Medical Institute

American Heart Association

U.S. Department of Energy

Biological and Environmental Research

Publisher

Oxford University Press (OUP)

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