Bacterial Argonaute nucleases reveal different modes of DNA targeting in vitro and in vivo

Author:

Lisitskaya Lidiya12,Kropocheva Ekaterina12,Agapov Aleksei2ORCID,Prostova Maria12,Panteleev Vladimir123ORCID,Yudin Denis2,Ryazansky Sergei2ORCID,Kuzmenko Anton24,Aravin Alexei A4,Esyunina Daria12ORCID,Kulbachinskiy Andrey12ORCID

Affiliation:

1. Institute of Gene Biology, Russian Academy of Sciences , Moscow 119334 , Russia

2. Institute of Molecular Genetics, National Research Center “Kurchatov Institute” , Moscow 123182 , Russia

3. Moscow Institute of Physics and Technology , Dolgoprudny 141700 , Russia

4. Division of Biology and Biological Engineering, California Institute of Technology , Pasadena , CA 91125, USA

Abstract

Abstract Prokaryotic Argonaute proteins (pAgos) are homologs of eukaryotic Argonautes (eAgos) and are also thought to play a role in cell defense against invaders. However, pAgos are much more diverse than eAgos and little is known about their functional activities and target specificities in vivo. Here, we describe five pAgos from mesophilic bacteria that act as programmable DNA endonucleases and analyze their ability to target chromosomal and invader DNA. In vitro, the analyzed proteins use small guide DNAs for precise cleavage of single-stranded DNA at a wide range of temperatures. Upon their expression in Escherichia coli, all five pAgos are loaded with small DNAs preferentially produced from plasmids and chromosomal regions of replication termination. One of the tested pAgos, EmaAgo from Exiguobacterium marinum, can induce DNA interference between homologous sequences resulting in targeted processing of multicopy plasmid and genomic elements. EmaAgo also protects bacteria from bacteriophage infection, by loading phage-derived guide DNAs and decreasing phage DNA content and phage titers. Thus, the ability of pAgos to target multicopy elements may be crucial for their protective function. The wide spectrum of pAgo activities suggests that they may have diverse functions in vivo and paves the way for their use in biotechnology.

Funder

Ministry of Science and Higher Education

Russian Science Foundation

Publisher

Oxford University Press (OUP)

Subject

Genetics

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