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

bioRxiv : the preprint server for biology · 2023

Abstract

Large-genome bacteriophages (jumbo phages) of the <i>Chimalliviridae</i> family assemble a nucleus-like compartment bounded by a protein shell that protects the replicating phage genome from host-encoded restriction enzymes and 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 <i>in vitro</i>, and binds phage mRNAs in infected cells. ChmC also forms phase-separated condensates with RNA <i>in vitro</i>. Targeted knockdown of ChmC using mRNA-targeting dCas13d halts infections at an early stage. Taken together, our data suggest that the conserved ChmC protein acts as a chaperone for phage mRNAs, potentially stabilizing these mRNAs and driving their translocation through the nuclear shell to promote translation and infection progression.

Publication Types

["Preprint", "Journal Article"]

Keywords

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MeSH Terms

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Funding

R01 HG004659 NHGRI NIH HHS (United States)
R35 GM144121 NIGMS NIH HHS (United States)
S10 OD021724 NIH HHS (United States)
R01 GM129245 NIGMS NIH HHS (United States)