Abstract

This competitive renewal application proposes a continuation of the Stanford Genome Training Program (SGTP), one of the first NHGRI-sponsored genome training programs established six years ago. Building on the highly-successful program that has supported and trained 48 Graduate Student and Postdoctoral Fellow Trainees in 20 funded slots during this first funding period, the proposed continuation will expand to 32 Graduate Student slots and 4 Postdoctoral Fellow slots. These Trainees will work in the laboratories of 35 Participating Faculty members in 12 different Departments on the Stanford campus on a very wide array of genomics projects, including DNA and protein microarray experiments, large-scale sequencing and mapping of genomes, comparative sequencing and analysis, functional genomics, statistical genetics and genomics, highthroughput genotyping and genetic analysis, evolutionary genomics, pharmacogenetics, developmental biology and many other biological problems that benefit from a genomics perspective. The SGTP will continue to have a strong computational and quantitative component, with more than a third of the Trainees doing purely computational and analytical research and essentially all of the others using tools developed by bioinformatics researchers. Trainees will have a structured training plan administered by a dedicated Executive Committee comprised of the Principal Investigator/Program Director and four additional Participating Faculty members. This plan includes a regular series of Trainee research talks, a Genomics Seminar Series, Trainee-specific coursework plans developed by the Executive Committee with each Trainee, and a yearly Genomics Lectureship designed and run by the Trainees. Trainees and Participating Faculty will participate in a number of activities designed to recruit and teach individuals who are members of under-represented minorities, and to extend the genomics message to fellow scientists and non-scientists at a range of age levels.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Human Genome Research Institute (NHGRI)
Type
Institutional National Research Service Award (T32)
Project #
5T32HG000044-07
Application #
6662624
Study Section
Special Emphasis Panel (ZHG1-HGR-P (M1))
Program Officer
Graham, Bettie
Project Start
1995-09-01
Project End
2007-08-31
Budget Start
2003-09-30
Budget End
2004-08-31
Support Year
7
Fiscal Year
2003
Total Cost
$1,513,435
Indirect Cost

  Institution

Name
Stanford University
Department
Genetics
Type
Schools of Medicine
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Zhang, Haiyang; Wang, Yi; Bai, Ming et al. (2018) Exosomes serve as nanoparticles to suppress tumor growth and angiogenesis in gastric cancer by delivering hepatocyte growth factor siRNA. Cancer Sci 109:629-641
Garcia, Victor; Glassberg, Emily C; Harpak, Arbel et al. (2018) Clonal interference can cause wavelet-like oscillations of multilocus linkage disequilibrium. J R Soc Interface 15:
Gowans, Graeme J; Schep, Alicia N; Wong, Ka Man et al. (2018) INO80 Chromatin Remodeling Coordinates Metabolic Homeostasis with Cell Division. Cell Rep 22:611-623
Kovary, Kyle M; Taylor, Brooks; Zhao, Michael L et al. (2018) Expression variation and covariation impair analog and enable binary signaling control. Mol Syst Biol 14:e7997
Cho, Seung Woo; Xu, Jin; Sun, Ruping et al. (2018) Promoter of lncRNA Gene PVT1 Is a Tumor-Suppressor DNA Boundary Element. Cell 173:1398-1412.e22
Beckwith, Sean L; Schwartz, Erin K; GarcĂ­a-Nieto, Pablo E et al. (2018) The INO80 chromatin remodeler sustains metabolic stability by promoting TOR signaling and regulating histone acetylation. PLoS Genet 14:e1007216
Breslow, David K; Hoogendoorn, Sascha; Kopp, Adam R et al. (2018) A CRISPR-based screen for Hedgehog signaling provides insights into ciliary function and ciliopathies. Nat Genet 50:460-471
Buenrostro, Jason D; Corces, M Ryan; Lareau, Caleb A et al. (2018) Integrated Single-Cell Analysis Maps the Continuous Regulatory Landscape of Human Hematopoietic Differentiation. Cell 173:1535-1548.e16
Ofir, Gal; Melamed, Sarah; Sberro, Hila et al. (2018) DISARM is a widespread bacterial defence system with broad anti-phage activities. Nat Microbiol 3:90-98
Deng, Tanggang; Yan, Guobei; Song, Xin et al. (2018) Deubiquitylation and stabilization of p21 by USP11 is critical for cell-cycle progression and DNA damage responses. Proc Natl Acad Sci U S A 115:4678-4683

Showing the most recent 10 out of 327 publications