Author
Listed:
- Fabio Puddu
(University of Cambridge
University of Cambridge
Wellcome Sanger Institute)
- Mareike Herzog
(University of Cambridge
University of Cambridge
Wellcome Sanger Institute)
- Alexandra Selivanova
(University of Cambridge
University of Cambridge)
- Siyue Wang
(University of Cambridge
University of Cambridge)
- Jin Zhu
(Johns Hopkins University School of Medicine)
- Shir Klein-Lavi
(Tel Aviv University)
- Molly Gordon
(Johns Hopkins University School of Medicine)
- Roi Meirman
(Tel Aviv University)
- Gonzalo Millan-Zambrano
(University of Cambridge
University of Cambridge)
- Iñigo Ayestaran
(University of Cambridge
University of Cambridge)
- Israel Salguero
(University of Cambridge
University of Cambridge)
- Roded Sharan
(Tel Aviv University)
- Rong Li
(Johns Hopkins University School of Medicine)
- Martin Kupiec
(Tel Aviv University)
- Stephen P. Jackson
(University of Cambridge
University of Cambridge)
Abstract
Despite major progress in defining the functional roles of genes, a complete understanding of their influences is far from being realized, even in relatively simple organisms. A major milestone in this direction arose via the completion of the yeast Saccharomyces cerevisiae gene-knockout collection (YKOC), which has enabled high-throughput reverse genetics, phenotypic screenings and analyses of synthetic-genetic interactions1–3. Ensuing experimental work has also highlighted some inconsistencies and mistakes in the YKOC, or genome instability events that rebalance the effects of specific knockouts4–6, but a complete overview of these is lacking. The identification and analysis of genes that are required for maintaining genomic stability have traditionally relied on reporter assays and on the study of deletions of individual genes, but whole-genome-sequencing technologies now enable—in principle—the direct observation of genome instability globally and at scale. To exploit this opportunity, we sequenced the whole genomes of nearly all of the 4,732 strains comprising the homozygous diploid YKOC. Here, by extracting information on copy-number variation of tandem and interspersed repetitive DNA elements, we describe—for almost every single non-essential gene—the genomic alterations that are induced by its loss. Analysis of this dataset reveals genes that affect the maintenance of various genomic elements, highlights cross-talks between nuclear and mitochondrial genome stability, and shows how strains have genetically adapted to life in the absence of individual non-essential genes.
Suggested Citation
Fabio Puddu & Mareike Herzog & Alexandra Selivanova & Siyue Wang & Jin Zhu & Shir Klein-Lavi & Molly Gordon & Roi Meirman & Gonzalo Millan-Zambrano & Iñigo Ayestaran & Israel Salguero & Roded Sharan &, 2019.
"Genome architecture and stability in the Saccharomyces cerevisiae knockout collection,"
Nature, Nature, vol. 573(7774), pages 416-420, September.
Handle:
RePEc:nat:nature:v:573:y:2019:i:7774:d:10.1038_s41586-019-1549-9
DOI: 10.1038/s41586-019-1549-9
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