Haploid yeast cells undergo a reversible phenotypic switch associated with chromosome II copy number

Drozdova, Polina; Mironova, L. N.; Zhouravleva, Galina A.

doi:10.1186/s12863-016-0464-4

Cited by 10 publications

(7 citation statements)

References 49 publications

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“…Recent years have seen a huge amount of published S. cerevisiae genome sequences, which have revealed a high level of genetic diversity, phenotypic variation and copy number variation in this species [ 24 , 37 , 38 , 39 , 40 ]. In some of the works, it has been shown that structural changes in the genome (such as CNVs) may have an adaptive role (e.g., [ 38 ]), however, it remains unclear if selective pressure may actively facilitate the accumulation of genetic changes.…”

Section: Discussionmentioning

confidence: 99%

“…Previously, several similar observations of aneuploidies associated with nonsense suppression and release factor genes have been reported. These include a phenomenon of reversible nonsense suppressor phenotype switching due to chromosome II copy number observed in the presence of missense mutations in the SUP35 and SUP45 genes [ 40 ]. This case is reminiscent of the chromosome II disomy, which we observed in this work in the sup35-203 mutant.…”

Section: Discussionmentioning

confidence: 99%

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Gene Amplification as a Mechanism of Yeast Adaptation to Nonsense Mutations in Release Factor Genes

Maksiutenko

Barbitoff

Matveenko

et al. 2021

Genes

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Protein synthesis (translation) is one of the fundamental processes occurring in the cells of living organisms. Translation can be divided into three key steps: initiation, elongation, and termination. In the yeast Saccharomyces cerevisiae, there are two translation termination factors, eRF1 and eRF3. These factors are encoded by the SUP45 and SUP35 genes, which are essential; deletion of any of them leads to the death of yeast cells. However, viable strains with nonsense mutations in both the SUP35 and SUP45 genes were previously obtained in several groups. The survival of such mutants clearly involves feedback control of premature stop codon readthrough; however, the exact molecular basis of such feedback control remain unclear. To investigate the genetic factors supporting the viability of these SUP35 and SUP45 nonsense mutants, we performed whole-genome sequencing of strains carrying mutant sup35-n and sup45-n alleles; while no common SNPs or indels were found in these genomes, we discovered a systematic increase in the copy number of the plasmids carrying mutant sup35-n and sup45-n alleles. We used the qPCR method which confirmed the differences in the relative number of SUP35 and SUP45 gene copies between strains carrying wild-type or mutant alleles of SUP35 and SUP45 genes. Moreover, we compare the number of copies of the SUP35 and SUP45 genes in strains carrying different nonsense mutant variants of these genes as a single chromosomal copy. qPCR results indicate that the number of mutant gene copies is increased compared to the wild-type control. In case of several sup45-n alleles, this was due to a disomy of the entire chromosome II, while for the sup35-218 mutation we observed a local duplication of a segment of chromosome IV containing the SUP35 gene. Taken together, our results indicate that gene amplification is a common mechanism of adaptation to nonsense mutations in release factor genes in yeast.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Gene Amplification as a Mechanism of Yeast Adaptation to Nonsense Mutations in Release Factor Genes

Maksiutenko

Barbitoff

Matveenko

et al. 2021

Genes

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“…Thus, the chromosome I disomy may potentially alleviate this process by increasing ade1-14 levels, which was previously found to compensate for the growth defects of the strains with the same genotype on a media without adenine [43]. Notably, the aneuploidy was demonstrated to be associated with the formation of different non-chromosomal determinants affecting the translation termination efficiency, like [ ISP + ] (initially described as a prion form of the transcriptional regulator Sfp1 [11] and later connected with the chromosome II copy number [69]), as well as the [ ASP + ] (chromosome VIII disomy [70]). Probably, the prion formation by several proteins regulating key biological processes could induce genome instability in a few fractions of cells that are inherited by progeny under selective pressure and determine adaptive phenotypic traits like resistance to poisonous compounds.…”

Section: Discussionmentioning

confidence: 99%

RNA Sequencing Reveals Specific Transcriptomic Signatures Distinguishing Effects of the [SWI+] Prion and SWI1 Deletion in Yeast Saccharomyces cerevisiae

Malovichko

Antonets

Maslova

et al. 2019

Genes

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Prions are infectious, self-perpetuating protein conformers. In mammals, pathological aggregation of the prion protein causes incurable neurodegenerative disorders, while in yeast Saccharomyces cerevisiae, prion formation may be neutral or even beneficial. According to the prevailing contemporary point of view, prion formation is considered to be a functional inactivation of the corresponding protein whose conformational state shifts from the functional monomeric one to the infectious aggregated one. The Swi1 protein forms the [SWI+] prion and belongs to the nucleosome remodeler complex SWI/SNF controlling the expression of a significant part of the yeast genome. In this work, we performed RNA sequencing of isogenic S. cerevisiae strains grown on the media containing galactose as the sole carbon source. These strains bore the [SWI+] prion or had its structural gene SWI1 deleted. The comparative analysis showed that [SWI+] affects genome expression significantly weaker as compared to the SWI1 deletion. Moreover, in contrast to [SWI+], the SWI1 deletion causes the general inhibition of translation-related genes expression and chromosome I disomy. At the same time, the [SWI+] prion exhibits a specific pattern of modulation of the metabolic pathways and some biological processes and functions, as well as the expression of several genes. Thus, the [SWI+] prion only partially corresponds to the loss-of-function of SWI1 and demonstrates several gain-of-function traits.

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“…Custom 8x15k design (AMID 028943) Agilent arrays were used. CGH analysis was carried out as described previously ( Drozdova et al 2016a ). The data were processed with the CGH-Miner Excel add-in ( Wang et al, 2005 ) and a custom R function based on the clac package.…”

Section: Methodsmentioning

confidence: 99%

Chromosome-level genome assembly and structural variant analysis of two laboratory yeast strains from the Peterhof Genetic Collection lineage

Barbitoff

Matveenko

Matiiv

et al. 2021

G3 Genes|Genomes|Genetics

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Thousands of yeast genomes have been sequenced with both traditional and long-read technologies, and multiple observations about modes of genome evolution for both wild and laboratory strains have been drawn from these sequences. In our study, we applied Oxford Nanopore and Illumina technologies to assemble complete genomes of two widely used members of a distinct laboratory yeast lineage, the Peterhof Genetic Collection (PGC), and investigate the structural features of these genomes including transposable element content, copy number alterations, and structural rearrangements. We identified numerous notable structural differences between genomes of PGC strains and the reference S288C strain. We discovered a substantial enrichment of mid-length insertions and deletions within repetitive coding sequences, such as in the SCH9 gene or the NUP100 gene, with possible impact of these variants on protein amyloidogenicity. High contiguity of the final assemblies allowed us to trace back the history of reciprocal unbalanced translocations between chromosomes I, VIII, IX, XI, and XVI of the PGC strains. We show that formation of hybrid alleles of the FLO genes during such chromosomal rearrangements is likely responsible for the lack of invasive growth of yeast strains. Taken together, our results highlight important features of laboratory yeast strain evolution using the power of long-read sequencing.

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Haploid yeast cells undergo a reversible phenotypic switch associated with chromosome II copy number

Cited by 10 publications

References 49 publications

Gene Amplification as a Mechanism of Yeast Adaptation to Nonsense Mutations in Release Factor Genes

Gene Amplification as a Mechanism of Yeast Adaptation to Nonsense Mutations in Release Factor Genes

RNA Sequencing Reveals Specific Transcriptomic Signatures Distinguishing Effects of the [SWI+] Prion and SWI1 Deletion in Yeast Saccharomyces cerevisiae

Chromosome-level genome assembly and structural variant analysis of two laboratory yeast strains from the Peterhof Genetic Collection lineage

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