Advancing the Genetic Engineering Toolbox by Combining AsCas12a Knock-in Mice with Ultra-compact Screening

Overview

Journal Nat Commun

Date 2025 Jan 30

PMID 39885149

Authors

Wei Jin

Yexuan Deng

John E La Marca

Emily J Lelliott

Sarah T Diepstraten

Christina Konig

Lin Tai

Valentina Snetkova

Kristel M Dorighi

Luke Hoberecht

Millicent G Hedditch

Lauren Whelan

Geraldine Healey

Dan Fayle

Kieran Lau

Margaret A Potts

Moore Z Chen

Angus P R Johnston

Yang Liao

Wei Shi

Andrew J Kueh

Benjamin Haley

Jean-Philippe Fortin

Marco J Herold

Affiliations

Soon will be listed here.

Abstract

Cas12a is a next-generation gene editing tool that enables multiplexed gene targeting. Here, we present a mouse model that constitutively expresses enhanced Acidaminococcus sp. Cas12a (enAsCas12a) linked to an mCherry fluorescent reporter. We demonstrate efficient single and multiplexed gene editing in vitro, using primary and transformed cells from enAsCas12a mice. We further demonstrate successful in vivo gene editing, using normal and cancer-prone enAsCas12a stem cells to reconstitute the haematopoietic system of wild-type mice. We also present compact, genome-wide Cas12a knockout libraries, with four crRNAs per gene encoded across one (Scherzo) or two (Menuetto) vectors, and demonstrate the utility of these libraries across methodologies: in vitro enrichment and drop-out screening in lymphoma cells and immortalised fibroblasts, respectively, and in vivo screens to identify lymphoma-driving events. Finally, we demonstrate CRISPR multiplexing via simultaneous gene knockout (via Cas12a) and activation (via dCas9-SAM) using primary T cells and fibroblasts. Our enAsCas12a mouse and accompanying crRNA libraries enhance genome engineering capabilities and complement current CRISPR technologies.

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