A compact Cas9 ortholog from Staphylococcus Auricularis (SauriCas9) expands the DNA targeting scope

Ziying Hu; Shuai Wang; Chengdong Zhang; Ning Gao; Miaomiao Li; Deqian Wang; Daqi Wang; Dong Liu; Huihui Liu; Sang‐Ging Ong; Hongyan Wang; Yongming Wang

doi:10.1371/journal.pbio.3000686

A compact Cas9 ortholog from Staphylococcus Auricularis (SauriCas9) expands the DNA targeting scope

Ziying Hu(Fudan University), Shuai Wang(Fudan University), Chengdong Zhang(Fudan University), Ning Gao(Fudan University), Miaomiao Li(Fudan University), Deqian Wang(Fudan University), Daqi Wang(Fudan University), Dong Liu(Nantong University), Huihui Liu(Chinese Academy of Forestry), Sang‐Ging Ong(University of Illinois Urbana-Champaign), Hongyan Wang(Fudan University), Yongming Wang(Nantong University)

PLoS Biology

March 30, 2020

10.1371/journal.pbio.3000686

Cited by 147Open Access

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Abstract

Compact CRISPR/Cas9 systems that can be packaged into an adeno-associated virus (AAV) hold great promise for gene therapy. Unfortunately, currently available small Cas9 nucleases either display low activity or require a long protospacer adjacent motif (PAM) sequence, limiting their extensive applications. Here, we screened a panel of Cas9 nucleases and identified a small Cas9 ortholog from Staphylococcus auricularis (SauriCas9), which recognizes a simple NNGG PAM, displays high activity for genome editing, and is compact enough to be packaged into an AAV for genome editing. Moreover, the conversion of adenine and cytosine bases can be achieved by fusing SauriCas9 to the cytidine and adenine deaminase. Therefore, SauriCas9 holds great potential for both basic research and clinical applications.

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