Abstract

To train predoctoral students in Neurobiology, 52 cooperating faculty propose continuation of broad, interdisciplinary predoctoral training program with approximately 63 total students in fall, 2001. These faculty members have research interests in molecular, cellular, developmental, systems, and medical neurobiology. They have appointments in several basic science and clinical departments with fully equipped, funded laboratories, mostly on the main UCSF campus at Parnassus Heights. We anticipate approximately 10 additional faculty will join our graduate program during the next five years. An annual retreat, a weekly seminar series, a weekly student-faculty journal club, and student journal/pizza club meetings will promote interactions benefiting trainees. Neuroscience training will be conducted within the broader context of the Boyer Program in Biological Sciences (P.I.B.S.), a consortium of 7 graduate programs with 185 total faculty. A weekly P.I.B.S. journal club, plus seminar series and retreats sponsored by the other P.I.B.S. programs will promote the broader education of our students and their interactions with the faculty and students of these programs. During the next 5 years, the number of our students at the beginning of each academic year is anticipated to be 60-70, increasing slowly from present size. We will continue major efforts to recruit under-represented minorities. The major selection criteria for all trainees will be originality, commitment and scientific potential. In the 1st year, students will take core courses in Neurobiology, Neuroanatomy, and Cell Biology and will rotate in 3 laboratories that will introduce them to major Neuroscience research areas. Later students will take at least four advanced seminar/discussion courses, exploring in depth subjects of particular importance. These will provide students will analytical skills, current knowledge and experience in making formal and informal scientific presentations. Near the end of the first year, trainees will chose Ph.D. thesis research mentors. During the 2nd year, the proposed thesis project will be described in a written proposal. During a qualifying examination, the importance, scope and feasibility of this project will be defended. The exam will also test knowledge and analytical abilities in broader areas of Neuroscience. Training in later years will focus on the research required for a Ph.D. thesis, but will be supplemented by seminars, conferences, and journal clubs. Our goal is to facilitate the intellectual growth and development of scientific skills of new investigators committed to solving major problems in Neuroscience and to making positive contributions to education in the 21st Century.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Institutional National Research Service Award (T32)
Project #
5T32GM007449-30
Application #
7077788
Study Section
National Institute of General Medical Sciences Initial Review Group (BRT)
Program Officer
Cole, Alison E
Project Start
1977-09-01
Project End
2007-06-30
Budget Start
2006-07-01
Budget End
2007-06-30
Support Year
30
Fiscal Year
2006
Total Cost
$306,161
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Physiology
Type
Schools of Medicine
DUNS #
094878337
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Clemente-Perez, Alexandra; Makinson, Stefanie Ritter; Higashikubo, Bryan et al. (2017) Distinct Thalamic Reticular Cell Types Differentially Modulate Normal and Pathological Cortical Rhythms. Cell Rep 19:2130-2142
Silberberg, Shanni N; Taher, Leila; Lindtner, Susan et al. (2016) Subpallial Enhancer Transgenic Lines: a Data and Tool Resource to Study Transcriptional Regulation of GABAergic Cell Fate. Neuron 92:59-74
Yuen, Tracy J; Silbereis, John C; Griveau, Amelie et al. (2014) Oligodendrocyte-encoded HIF function couples postnatal myelination and white matter angiogenesis. Cell 158:383-396
Gorczyca, David A; Younger, Susan; Meltzer, Shan et al. (2014) Identification of Ppk26, a DEG/ENaC Channel Functioning with Ppk1 in a Mutually Dependent Manner to Guide Locomotion Behavior in Drosophila. Cell Rep 9:1446-58
Pattabiraman, Kartik; Golonzhka, Olga; Lindtner, Susan et al. (2014) Transcriptional regulation of enhancers active in protodomains of the developing cerebral cortex. Neuron 82:989-1003
Silbereis, John C; Nobuta, Hiroko; Tsai, Hui-Hsin et al. (2014) Olig1 function is required to repress dlx1/2 and interneuron production in Mammalian brain. Neuron 81:574-87
McKinsey, Gabriel L; Lindtner, Susan; Trzcinski, Brett et al. (2013) Dlx1&2-dependent expression of Zfhx1b (Sip1, Zeb2) regulates the fate switch between cortical and striatal interneurons. Neuron 77:83-98
Visel, Axel; Taher, Leila; Girgis, Hani et al. (2013) A high-resolution enhancer atlas of the developing telencephalon. Cell 152:895-908
Seybold, Bryan A; Stanco, Amelia; Cho, Kathleen K A et al. (2012) Chronic reduction in inhibition reduces receptive field size in mouse auditory cortex. Proc Natl Acad Sci U S A 109:13829-34
Peterson, B E; Merzenich, M M (1995) EXP: a Macintosh program for automating data acquisition and analysis applied to neurophysiology. J Neurosci Methods 57:121-31

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