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Computationally designed hyperactive Cas9 enzymes
BiologyNature Communications

Computationally designed hyperactive Cas9 enzymes

P. D. Vos, G. Rossetti, et al.

This exciting research conducted by Pascal D. Vos, Giulia Rossetti, Jessica L. Mantegna, and others explores the engineering of hyperactive Cas9 enzymes, enhancing donor-independent editing activity. Using innovative computational design and yeast-based circuits, the study reveals significant improvements in CRISPR applications for broader genomic modifications.... show more
Abstract
The ability to alter the genomes of living cells is key to understanding how genes influence the functions of organisms and will be critical to modify living systems for useful purposes. However, this promise has long been limited by the technical challenges involved in genetic engineering. Recent advances in gene editing have bypassed some of these challenges but they are still far from ideal. Here we use FuncLib to computationally design Cas9 enzymes with substantially higher donor-independent editing activities. We use genetic circuits linked to cell survival in yeast to quantify Cas9 activity and discover synergistic interactions between engineered regions. These hyperactive Cas9 variants function efficiently in mammalian cells and introduce larger and more diverse pools of insertions and deletions into targeted genomic regions, providing tools to enhance and expand the possible applications of CRISPR-based gene editing.
Publisher
Nature Communications
Published On
May 31, 2022
Authors
Pascal D. Vos, Giulia Rossetti, Jessica L. Mantegna, Stefan J. Siira, Andrianto P. Gandadireja, Mitchell Bruce, Samuel A. Raven, Olga Khersonsky, Sarel J. Fleishman, Aleksandra Filipovska, Oliver Rackham
Tags
Cas9gene editingcomputational designmutationsCRISPRmammalian cellsgenomic sites
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