Abstract

The long-term goal of this proposed collaborative project is to define the structural basis and mechanistic? principles of systems that mediate information flow essential for virulence and persistence of Mycobacterium? tuberculosis (Mtb). Within the framework of the TB Structural Genomics Consortium (TBSGC), we will focus? structural, biochemical, computational, genetic and microarray methods on four processes?DMA replication? and repair, transcription, phospho-Ser/Thr/Tyr signaling and sulfur metabolism. This research has four? specific aims:? 1. Define the structures and functions of Mtb proteins that mediate DMA replication and repair.? 2. Determine the structures and mechanisms of inhibition of Mtb RNA polymerase, the Rho transcription? termination factor and several RNases.? 3. Determine the structures and signaling pathways of Ser/Thr kinases and protein tyrosine phosphatases? in Mtb.? 4. Establish the structures and the roles sulfotransfer enzymes in Mtb growth and persistence.? The genomic perspective and broad attack needed to achieve these aims rest on strong collaborations with? the other TBSGC components. The Core Facilities for Cloning and Protein Production will make many? expression vectors and proteins for analysis. The crystallization core facilities will identify crystallization? conditions, and the Data Collection Core will provide essential data for rapid structure determination.? Microarray experiments in this project will help identify pathways and targets for all TBSGC components.? Project 1 will use selected high-resolution structures for collaborative virtual screens for inhibitors. We will? collaborate with the other Projects to analyze the structures and functions of key phosphorylated proteins.? Coordination requires the TBSGC web site (Project 2) and administrative framework.? This project and the TBSGC as a whole have high significance for human health. Mtb infects one third of the? world's population and annually kills over two million people worldwide. By revealing how signals regulate? Mtb metabolism and defining the mechanisms of antibiotic and inhibitor binding, this project will stimulate? development of new therapeutics to efficiently cure persistent Mtb infections.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI068135-02
Application #
7506328
Study Section
Special Emphasis Panel (ZAI1)
Project Start
Project End
Budget Start
2007-04-01
Budget End
2008-03-31
Support Year
2
Fiscal Year
2007
Total Cost
$469,470
Indirect Cost

  Institution

Name
Texas Agrilife Research
Department
Type
DUNS #
847205713
City
College Station
State
TX
Country
United States
Zip Code
77843

  Publications

Tuukkanen, Anne T; Freire, Diana; Chan, Sum et al. (2018) Structural Variability of EspG Chaperones from Mycobacterial ESX-1, ESX-3, and ESX-5 Type VII Secretion Systems. J Mol Biol :
Prigozhin, Daniil M; Papavinasasundaram, Kadamba G; Baer, Christina E et al. (2016) Structural and Genetic Analyses of the Mycobacterium tuberculosis Protein Kinase B Sensor Domain Identify a Potential Ligand-binding Site. J Biol Chem 291:22961-22969
Wagner, Jonathan M; Chan, Sum; Evans, Timothy J et al. (2016) Structures of EccB1 and EccD1 from the core complex of the mycobacterial ESX-1 type VII secretion system. BMC Struct Biol 16:5
DeJesus, Michael A; Zhang, Yanjia J; Sassetti, Christopher M et al. (2013) Bayesian analysis of gene essentiality based on sequencing of transposon insertion libraries. Bioinformatics 29:695-703
Liu, Zhen; Ioerger, Thomas R; Wang, Feng et al. (2013) Structures of Mycobacterium tuberculosis FadD10 protein reveal a new type of adenylate-forming enzyme. J Biol Chem 288:18473-83
Ioerger, Thomas R; O'Malley, Theresa; Liao, Reiling et al. (2013) Identification of new drug targets and resistance mechanisms in Mycobacterium tuberculosis. PLoS One 8:e75245
Miallau, Linda; Jain, Paras; Arbing, Mark A et al. (2013) Comparative proteomics identifies the cell-associated lethality of M. tuberculosis RelBE-like toxin-antitoxin complexes. Structure 21:627-37
Tretter, Elsa M; Berger, James M (2012) Mechanisms for defining supercoiling set point of DNA gyrase orthologs: II. The shape of the GyrA subunit C-terminal domain (CTD) is not a sole determinant for controlling supercoiling efficiency. J Biol Chem 287:18645-54
Chim, Nicholas; Owens, Cedric P; Contreras, Heidi et al. (2012) Advances In Mycobacterium Tuberculosis Therapeutics Discovery Utlizing Structural Biology. Infect Disord Drug Targets :
Cavazos, Alexandra; Prigozhin, Daniil M; Alber, Tom (2012) Structure of the sensor domain of Mycobacterium tuberculosis PknH receptor kinase reveals a conserved binding cleft. J Mol Biol 422:488-94

Showing the most recent 10 out of 51 publications