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CRI-SPA: a high-throughput method for systematic genetic editing of yeast libraries

Authors :
Cachera, Paul
Olsson, Helén
Coumou, Hilde
Jensen, Mads L
Sánchez, Benjamín J.
Strucko, Tomas
van den Broek, Marcel
Daran, Jean-Marc
Jensen, Michael K.
Sonnenschein, Nikolaus
Lisby, Michael
Mortensen, Uffe H.
Cachera, Paul
Olsson, Helén
Coumou, Hilde
Jensen, Mads L
Sánchez, Benjamín J.
Strucko, Tomas
van den Broek, Marcel
Daran, Jean-Marc
Jensen, Michael K.
Sonnenschein, Nikolaus
Lisby, Michael
Mortensen, Uffe H.
Source :
Cachera , P , Olsson , H , Coumou , H , Jensen , M L , Sánchez , B J , Strucko , T , van den Broek , M , Daran , J-M , Jensen , M K , Sonnenschein , N , Lisby , M & Mortensen , U H 2023 , ' CRI-SPA: a high-throughput method for systematic genetic editing of yeast libraries ' , Nucleic Acids Research , vol. 51 , no. 17 , e91 .
Publication Year :
2023

Abstract

Biological functions are orchestrated by intricate networks of interacting genetic elements. Predicting the interaction landscape remains a challenge for systems biology and new research tools allowing simple and rapid mapping of sequence to function are desirable. Here, we describe CRI-SPA, a method allowing the transfer of chromosomal genetic features from a CRI-SPA Donor strain to arrayed strains in large libraries of Saccharomyces cerevisiae. CRI-SPA is based on mating, CRISPR-Cas9-induced gene conversion, and Selective Ploidy Ablation. CRI-SPA can be massively parallelized with automation and can be executed within a week. We demonstrate the power of CRI-SPA by transferring four genes that enable betaxanthin production into each strain of the yeast knockout collection (≈4800 strains). Using this setup, we show that CRI-SPA is highly efficient and reproducible, and even allows marker-free transfer of genetic features. Moreover, we validate a set of CRI-SPA hits by showing that their phenotypes correlate strongly with the phenotypes of the corresponding mutant strains recreated by reverse genetic engineering. Hence, our results provide a genome-wide overview of the genetic requirements for betaxanthin production. We envision that the simplicity, speed, and reliability offered by CRI-SPA will make it a versatile tool to forward systems-level understanding of biological processes.

Details

Database :
OAIster
Journal :
Cachera , P , Olsson , H , Coumou , H , Jensen , M L , Sánchez , B J , Strucko , T , van den Broek , M , Daran , J-M , Jensen , M K , Sonnenschein , N , Lisby , M & Mortensen , U H 2023 , ' CRI-SPA: a high-throughput method for systematic genetic editing of yeast libraries ' , Nucleic Acids Research , vol. 51 , no. 17 , e91 .
Notes :
application/pdf, English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1426749325
Document Type :
Electronic Resource