PpCas9 from Pasteurella pneumotropica — a compact Type II-C Cas9 ortholog active in human cells

Author:

Fedorova Iana12ORCID,Vasileva Aleksandra123,Selkova Polina123,Abramova Marina34,Arseniev Anatolii23,Pobegalov Georgii3,Kazalov Maksim34,Musharova Olga15,Goryanin Ignatiy1,Artamonova Daria1ORCID,Zyubko Tatyana3,Shmakov Sergey6,Artamonova Tatyana3,Khodorkovskii Mikhail3,Severinov Konstantin45ORCID

Affiliation:

1. Skolkovo Institute of Science and Technology, Center of Life Sciences, Moscow, 121205, Russia

2. Center for Precision Genome Editing and Genetic Technologies for Biomedicine, Institute of Gene Biology, Russian Academy of Sciences, Moscow, 119334, Russia

3. Peter the Great St. Petersburg Polytechnic University, Saint Petersburg, 195251, Russia

4. Saint Petersburg State University, Saint Petersburg, 199034, Russia

5. Institute of Molecular Genetics of National Research Center “Kurchatov Institute’’, Moscow, 123182, Russia

6. National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health, Bethesda, MD 20894, USA

Abstract

Abstract CRISPR-Cas defense systems opened up the field of genome editing due to the ease with which effector Cas nucleases can be programmed with guide RNAs to access desirable genomic sites. Type II-A SpCas9 from Streptococcus pyogenes was the first Cas9 nuclease used for genome editing and it remains the most popular enzyme of its class. Nevertheless, SpCas9 has some drawbacks including a relatively large size and restriction to targets flanked by an ‘NGG’ PAM sequence. The more compact Type II-C Cas9 orthologs can help to overcome the size limitation of SpCas9. Yet, only a few Type II-C nucleases were fully characterized to date. Here, we characterized two Cas9 II-C orthologs, DfCas9 from Defluviimonas sp.20V17 and PpCas9 from Pasteurella pneumotropica. Both DfCas9 and PpCas9 cleave DNA in vitro and have novel PAM requirements. Unlike DfCas9, the PpCas9 nuclease is active in human cells. This small nuclease requires an ‘NNNNRTT’ PAM orthogonal to that of SpCas9 and thus potentially can broaden the range of Cas9 applications in biomedicine and biotechnology.

Funder

Ministry of Science and Higher Education of the Russian Federation

Saint Petersburg State University

Publisher

Oxford University Press (OUP)

Subject

Genetics

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