Your search keyword '"Ye, Zirou"' showing total 4 results

1. The genomic diversification of grapevine clones.

Author

Vondras, Amanda, Figueroa-Balderas, Rosa, Penn, Michael, Zhou, Yongfeng, Ye, Zirou, Liang, Dingren, Espinoza, Lucero, Anderson, Michael, Walker, M, Gaut, Brandon, Cantu, Dario, Blanco-Ulate, Barbara, Seymour, Danelle, and Minio, Andrea

Subjects

Clonal propagation, DNA methylation, Genome diversification, Somatic mutations, Structural variation, Transposable elements, Clonal Evolution, DNA, Intergenic, Genome, Plant, Mutation, Vitis, Whole Genome Sequencing

Abstract

BACKGROUND: Vegetatively propagated clones accumulate somatic mutations. The purpose of this study was to better appreciate clone diversity and involved defining the nature of somatic mutations throughout the genome. Fifteen Zinfandel winegrape clone genomes were sequenced and compared to one another using a highly contiguous genome reference produced from one of the clones, Zinfandel 03. RESULTS: Though most heterozygous variants were shared, somatic mutations accumulated in individual and subsets of clones. Overall, heterozygous mutations were most frequent in intergenic space and more frequent in introns than exons. A significantly larger percentage of CpG, CHG, and CHH sites in repetitive intergenic space experienced transition mutations than in genic and non-repetitive intergenic spaces, likely because of higher levels of methylation in the region and because methylated cytosines often spontaneously deaminate. Of the minority of mutations that occurred in exons, larger proportions of these were putatively deleterious when they occurred in relatively few clones. CONCLUSIONS: These data support three major conclusions. First, repetitive intergenic space is a major driver of clone genome diversification. Second, clones accumulate putatively deleterious mutations. Third, the data suggest selection against deleterious variants in coding regions or some mechanism by which mutations are less frequent in coding than noncoding regions of the genome.

Published

2019

2. Red blotch disease alters grape berry development and metabolism by interfering with the transcriptional and hormonal regulation of ripening

Author

Blanco-Ulate, Barbara, Hopfer, Helene, Figueroa-Balderas, Rosa, Ye, Zirou, Rivero, Rosa M, Albacete, Alfonso, Pérez-Alfocea, Francisco, Koyama, Renata, Anderson, Michael M, Smith, Rhonda J, Ebeler, Susan E, and Cantu, Dario

Subjects

Genetics, 2.1 Biological and endogenous factors, Aetiology, Fruit, Geminiviridae, Gene Expression Profiling, Oligonucleotide Array Sequence Analysis, Plant Diseases, Vitis, Developmental regulation, metabolic flux, perennial woody crop, plant-virus interaction, secondary metabolism, veraison, viral disease, plant–virus interaction, véraison, Plant Biology, Crop and Pasture Production, Plant Biology & Botany

Abstract

Grapevine red blotch-associated virus (GRBaV) is a major threat to the wine industry in the USA. GRBaV infections (aka red blotch disease) compromise crop yield and berry chemical composition, affecting the flavor and aroma properties of must and wine. In this study, we combined genome-wide transcriptional profiling with targeted metabolite analyses and biochemical assays to characterize the impact of the disease on red-skinned berry ripening and metabolism. Using naturally infected berries collected from two vineyards, we were able to identify consistent berry responses to GRBaV across different environmental and cultural conditions. Specific alterations of both primary and secondary metabolism occurred in GRBaV-infected berries during ripening. Notably, GRBaV infections of post-véraison berries resulted in the induction of primary metabolic pathways normally associated with early berry development (e.g. thylakoid electron transfer and the Calvin cycle), while inhibiting ripening-associated pathways, such as a reduced metabolic flux in the central and peripheral phenylpropanoid pathways. We show that this metabolic reprogramming correlates with perturbations at multiple regulatory levels of berry development. Red blotch caused the abnormal expression of transcription factors (e.g. NACs, MYBs, and AP2-ERFs) and elements of the post-transcriptional machinery that function during red-skinned berry ripening. Abscisic acid, ethylene, and auxin pathways, which control both the initiation of ripening and stress responses, were also compromised. We conclude that GRBaV infections disrupt normal berry development and stress responses by altering transcription factors and hormone networks, which result in the inhibition of ripening pathways involved in the generation of color, flavor, and aroma compounds.

Published

2017

3. Developmental and Metabolic Plasticity of White-Skinned Grape Berries in Response to Botrytis cinerea during Noble Rot.

Author

Blanco-Ulate, Barbara, Amrine, Katherine CH, Collins, Thomas S, Rivero, Rosa M, Vicente, Ariel R, Morales-Cruz, Abraham, Doyle, Carolyn L, Ye, Zirou, Allen, Greg, Heymann, Hildegarde, Ebeler, Susan E, and Cantu, Dario

Subjects

Botrytis, Vitis, Fruit, Anthocyanins, Gene Expression Profiling, Plant Diseases, Gene Expression Regulation, Developmental, Gene Expression Regulation, Plant, Wine, Host-Pathogen Interactions, Metabolomics, Gene Expression Regulation, Developmental, Plant, Plant Biology & Botany, Biological Sciences, Agricultural and Veterinary Sciences

Abstract

Noble rot results from exceptional infections of ripe grape (Vitis vinifera) berries by Botrytis cinerea. Unlike bunch rot, noble rot promotes favorable changes in grape berries and the accumulation of secondary metabolites that enhance wine grape composition. Noble rot-infected berries of cv Sémillon, a white-skinned variety, were collected over 3 years from a commercial vineyard at the same time that fruit were harvested for botrytized wine production. Using an integrated transcriptomics and metabolomics approach, we demonstrate that noble rot alters the metabolism of cv Sémillon berries by inducing biotic and abiotic stress responses as well as ripening processes. During noble rot, B. cinerea induced the expression of key regulators of ripening-associated pathways, some of which are distinctive to the normal ripening of red-skinned cultivars. Enhancement of phenylpropanoid metabolism, characterized by a restricted flux in white-skinned berries, was a common outcome of noble rot and red-skinned berry ripening. Transcript and metabolite analyses together with enzymatic assays determined that the biosynthesis of anthocyanins is a consistent hallmark of noble rot in cv Sémillon berries. The biosynthesis of terpenes and fatty acid aroma precursors also increased during noble rot. We finally characterized the impact of noble rot in botrytized wines. Altogether, the results of this work demonstrated that noble rot causes a major reprogramming of berry development and metabolism. This desirable interaction between a fruit and a fungus stimulates pathways otherwise inactive in white-skinned berries, leading to a greater accumulation of compounds involved in the unique flavor and aroma of botrytized wines.

Published

2015

4. The genomic diversification of grapevine clones.

Author

Vondras, Amanda M, Vondras, Amanda M, Minio, Andrea, Blanco-Ulate, Barbara, Figueroa-Balderas, Rosa, Penn, Michael A, Zhou, Yongfeng, Seymour, Danelle, Ye, Zirou, Liang, Dingren, Espinoza, Lucero K, Anderson, Michael M, Walker, M Andrew, Gaut, Brandon, Cantu, Dario, Vondras, Amanda M, Vondras, Amanda M, Minio, Andrea, Blanco-Ulate, Barbara, Figueroa-Balderas, Rosa, Penn, Michael A, Zhou, Yongfeng, Seymour, Danelle, Ye, Zirou, Liang, Dingren, Espinoza, Lucero K, Anderson, Michael M, Walker, M Andrew, Gaut, Brandon, and Cantu, Dario

Abstract

BACKGROUND:Vegetatively propagated clones accumulate somatic mutations. The purpose of this study was to better appreciate clone diversity and involved defining the nature of somatic mutations throughout the genome. Fifteen Zinfandel winegrape clone genomes were sequenced and compared to one another using a highly contiguous genome reference produced from one of the clones, Zinfandel 03. RESULTS:Though most heterozygous variants were shared, somatic mutations accumulated in individual and subsets of clones. Overall, heterozygous mutations were most frequent in intergenic space and more frequent in introns than exons. A significantly larger percentage of CpG, CHG, and CHH sites in repetitive intergenic space experienced transition mutations than in genic and non-repetitive intergenic spaces, likely because of higher levels of methylation in the region and because methylated cytosines often spontaneously deaminate. Of the minority of mutations that occurred in exons, larger proportions of these were putatively deleterious when they occurred in relatively few clones. CONCLUSIONS:These data support three major conclusions. First, repetitive intergenic space is a major driver of clone genome diversification. Second, clones accumulate putatively deleterious mutations. Third, the data suggest selection against deleterious variants in coding regions or some mechanism by which mutations are less frequent in coding than noncoding regions of the genome.

Published

2019