Browsing by Author "Aydin, Selcan"

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    Different Mechanisms Confer Gradual Control and Memory at Nutrient- and Stress-Regulated Genes in Yeast.
    (Mol Cell Biol, 2015-11) Rienzo, Alessandro; Poveda-Huertes, Daniel; Aydin, Selcan; Buchler, Nicolas E; Pascual-Ahuir, Amparo; Proft, Markus
    Cells respond to environmental stimuli by fine-tuned regulation of gene expression. Here we investigated the dose-dependent modulation of gene expression at high temporal resolution in response to nutrient and stress signals in yeast. The GAL1 activity in cell populations is modulated in a well-defined range of galactose concentrations, correlating with a dynamic change of histone remodeling and RNA polymerase II (RNAPII) association. This behavior is the result of a heterogeneous induction delay caused by decreasing inducer concentrations across the population. Chromatin remodeling appears to be the basis for the dynamic GAL1 expression, because mutants with impaired histone dynamics show severely truncated dose-response profiles. In contrast, the GRE2 promoter operates like a rapid off/on switch in response to increasing osmotic stress, with almost constant expression rates and exclusively temporal regulation of histone remodeling and RNAPII occupancy. The Gal3 inducer and the Hog1 mitogen-activated protein (MAP) kinase seem to determine the different dose-response strategies at the two promoters. Accordingly, GAL1 becomes highly sensitive and dose independent if previously stimulated because of residual Gal3 levels, whereas GRE2 expression diminishes upon repeated stimulation due to acquired stress resistance. Our analysis reveals important differences in the way dynamic signals create dose-sensitive gene expression outputs.
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    Understanding the Effects of Genetic Variation on Osmo-adaptation Dynamics Across S. cerevisiae using Bulk Segregant Analysis and Whole Genome Sequencing
    (2017) Aydin, Selcan

    Adapting to environmental changes (i.e. an increase in osmolarity) is critical for cell survival. How cells respond and adapt to osmotic stress has been well-studied in the model eukaryote Saccharomyces cerevisiae. Although the molecular and systems properties of osmo-adaptation have been well studied, few studies have focused on the effects of genetic variation. Understanding how genetic variation affects molecular pathways and their dynamics, which translates to variation in cellular and organismal phenotypes, is a key step towards understanding important phenomena such as complex gene by gene interactions and the mapping of genotype to phenotype. The challenge is to causally connect genetic differences with cellular function and differences in complex traits between individuals. As a first step towards addressing this challenge, my dissertation research investigates how natural genetic variation affects osmo-adaptation dynamics in budding yeast, Saccharomyces cerevisiae.

    First, I characterized the natural variation in osmo-adaptation dynamics across S. cerevisiae. I showed that individual strains were highly variable in adaptation time and relative maximum growth rate after adapting to stress. Analysis of a broad set of genes involved in osmo-adaptation did not reveal any obvious genetic differences that could account for the observed variation. To identify alleles associated with the variation, I measured osmo-adaptation dynamics in progeny generated from a cross between two closely related lab strains. Identified alleles were outside the core signaling pathway and affected both adaptation time and relative maximum growth rate. Finally, I built a novel mapping panel and measured osmo-adaptation dynamics to obtain a more global, species-wide view. The panel showed an increased amount of variation in osmo-adaptation dynamics and a subset of progeny were phenotypically more extreme than their parents. Mapping the variation in this panel will generate a comprehensive list of alleles that affect osmo-adaptation. The strains in the mapping panel have a low number of mutations predicted to have strong effects in HOG pathway genes. Given our earlier results from the pairwise cross, I expect that many osmo-adaptation alleles discovered from the mapping panel will be outside the HOG pathway.