Abstract

Despite their importance in nearly all biological processes, the impacts of spatial and temporal effects on gene expression, protein abundance, and protein modification are greatly underrepresented in genome-wide analyses. This proposal is aimed at the development and implementation of new experimental and computational tools capable of measuring and modeling spatial and temporal biological data, focusing on the poorly studied relationship between the cell cycle and mitochondrial function in the model organism, S.cerevisiae. The research plan focuses on experimental systems for the large-scale measurement of mutant phenotype and genetic linkage, whole-genome RNA expression analysis using a system of RNA abundance, quantitation on an absolute scale, and mass spectrometry-based identification of proteins and protein modification states present in subcellular organelles. The computational analysis of this data will include the transcriptional regulatory network under these conditions, a model of yeast metabolism, and the relationship between evolution and organelle function. All of the techniques and methodologies developed in this study are designed to be genome-wide, high-throughput, cost-effective, and readily transferable to other systems. In addition to developing much needed technologies and computational tools, this project will also contribute important biological results that will further our understanding of previously characterized genes and pathways that are likely to be relevant to human disease. The candidate's long-term career goal is the establishment of an academic research laboratory focusing on the analysis of biological problems using a combination of functional genomics and computational modeling of biological processes. The Genome Scholar phase of the award will be used to improve computational skills and to acquire experience in the use of protein mass spectrometry. The Faculty Transition phase of the award will be used to establish a multidisciplinary environment for the conduct of genomics research.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Human Genome Research Institute (NHGRI)
Type
Career Transition Award (K22)
Project #
5K22HG002908-05
Application #
7523918
Study Section
Ethical, Legal, Social Implications Review Committee (GNOM)
Program Officer
Feingold, Elise A
Project Start
2003-08-15
Project End
2009-10-31
Budget Start
2008-11-01
Budget End
2009-10-31
Support Year
5
Fiscal Year
2009
Total Cost
$270,000
Indirect Cost

  Institution

Name
Institute for Systems Biology
Department
Type
DUNS #
135646524
City
Seattle
State
WA
Country
United States
Zip Code
98109

  Publications

Cary, Gregory A; Vinh, Dani B N; May, Patrick et al. (2015) Proteomic Analysis of Dhh1 Complexes Reveals a Role for Hsp40 Chaperone Ydj1 in Yeast P-Body Assembly. G3 (Bethesda) 5:2497-511
Scott, Adrian C; Ludlow, Catherine L; Cromie, Gareth A et al. (2014) BEST: barcode enabled sequencing of tetrads. J Vis Exp :
Cromie, Gareth A; Hyma, Katie E; Ludlow, Catherine L et al. (2013) Genomic sequence diversity and population structure of Saccharomyces cerevisiae assessed by RAD-seq. G3 (Bethesda) 3:2163-71
Ludlow, Catherine L; Scott, Adrian C; Cromie, Gareth A et al. (2013) High-throughput tetrad analysis. Nat Methods 10:671-5
Ruusuvuori, Pekka; Aijo, Tarmo; Chowdhury, Sharif et al. (2010) Evaluation of methods for detection of fluorescence labeled subcellular objects in microscope images. BMC Bioinformatics 11:248
Lee, Su-In; Dudley, Aimée M; Drubin, David et al. (2009) Learning a prior on regulatory potential from eQTL data. PLoS Genet 5:e1000358
Snitkin, Evan S; Dudley, Aimee M; Janse, Daniel M et al. (2008) Model-driven analysis of experimentally determined growth phenotypes for 465 yeast gene deletion mutants under 16 different conditions. Genome Biol 9:R140