Abstract

The parent P41 Center grant (5 P41 RR001209, A Synchrotron Radiation Structural Biology Resource, K.O. Hodgson, P.l.) has as its overall aim to develop new and enhanced approaches for the investigation of biomolecular structure and function using synchrotron radiation at Stanford Synchrotron Radiation Lightsource (SSRL). One of the Center's three methodologies and technical research and development (TR&D) areas is macromolecular crystallography. Since the submission of the competitive renewal in May, 2009, a revolutionary new x-ray light source has become available that could well have a transformative impact in macromolecular crystallography (and other areas of structural biology). This light source, an x-ray free electron laser named LCLS, located at the SLAC National Accelerator Laboratory (and in close proximity to SSRL) is now in full operation. Several key proof-of-principle experiments have been carried out and published, demonstrating the feasibility of obtaining high quality, potentially radiation damage free diffraction data from nanocrystals. Data on such samples cannot be obtained from any other source. There are several key technical R&D areas, which need to be addressed, and problems that need to be solved, for this innovative new approach to be successful and applicable to important biomedical problems and made widely available to the biomedical research community. Three TR&D areas are the focus of this Revision Application, in response to the NIH FOA PAR-12-046. The P41 Center, in close partnership with the LCLS scientific team and with the Physical Biosciences Division at Lawrence Berkeley National Laboratory (LBNL) will build upon existing core capabilities, augmented with proposed staff and instrumentation, to address nanocrystal growth, characterization and manipulation, data reduction and analysis, and structure solution, to provide an integrated capability for nanocrystallography using the LCLS. Also key is significant integration with specific facilities and beam lines at SSRL for technology development and characterization. The TR&D projects will be driven strongly by research collaborations (Driving Biomedical Projects).

Public Health Relevance

As with the parent grant and Center, relevance is to a number of important biological problems including membrane-bound proteins such as G-coupled receptors;the structure of metalloproteins involved in metabolism;and how these structures change in different states or evolve in time. Such information is more broadly important to the health-related areas of drug discovery, cancer research, and cell development.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Biotechnology Resource Grants (P41)
Project #
3P41GM103393-33S1
Application #
8416519
Study Section
Special Emphasis Panel (ZRG1-BCMB-P (40))
Program Officer
Swain, Amy L
Project Start
1997-03-01
Project End
2015-02-28
Budget Start
2012-08-15
Budget End
2013-02-28
Support Year
33
Fiscal Year
2012
Total Cost
$250,000
Indirect Cost
$32,241

  Institution

Name
Stanford University
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
009214214
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Jackson, David R; Shakya, Gaurav; Patel, Avinash B et al. (2018) Structural and Functional Studies of the Daunorubicin Priming Ketosynthase DpsC. ACS Chem Biol 13:141-151
Sibener, Leah V; Fernandes, Ricardo A; Kolawole, Elizabeth M et al. (2018) Isolation of a Structural Mechanism for Uncoupling T Cell Receptor Signaling from Peptide-MHC Binding. Cell 174:672-687.e27
Jennings, Gareth K; Hsu, Mei-Hui; Shock, Lisa S et al. (2018) Noncovalent interactions dominate dynamic heme distortion in cytochrome P450 4B1. J Biol Chem 293:11433-11446
Bowden, Catherine F M; Chan, Anson C K; Li, Emily J W et al. (2018) Structure-function analyses reveal key features in Staphylococcus aureus IsdB-associated unfolding of the heme-binding pocket of human hemoglobin. J Biol Chem 293:177-190
Moon, Thomas M; D'Andréa, Éverton D; Lee, Christopher W et al. (2018) The structures of penicillin-binding protein 4 (PBP4) and PBP5 from Enterococci provide structural insights into ?-lactam resistance. J Biol Chem 293:18574-18584
Fan, Ruixi; Serrano-Plana, Joan; Oloo, Williamson N et al. (2018) Spectroscopic and DFT Characterization of a Highly Reactive Nonheme FeV-Oxo Intermediate. J Am Chem Soc 140:3916-3928
Chiang, Linus; Wasinger, Erik C; Shimazaki, Yuichi et al. (2018) Electronic Structure and Reactivity Studies of a Nonsymmetric One-Electron Oxidized CuII Bis-phenoxide Complex. Inorganica Chim Acta 481:151-158
Moon, Thomas M; Sheehe, Jessica L; Nukareddy, Praveena et al. (2018) An N-terminally truncated form of cyclic GMP-dependent protein kinase I? (PKG I?) is monomeric and autoinhibited and provides a model for activation. J Biol Chem 293:7916-7929
Bitra, Aruna; Doukov, Tzanko; Wang, Jing et al. (2018) Crystal structure of murine 4-1BB and its interaction with 4-1BBL support a role for galectin-9 in 4-1BB signaling. J Biol Chem 293:1317-1329
Laursen, Nick S; Friesen, Robert H E; Zhu, Xueyong et al. (2018) Universal protection against influenza infection by a multidomain antibody to influenza hemagglutinin. Science 362:598-602

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