In the past several years, our work has concentrated in four distinct areas. Crystallographic studies of proteases Crystallographic studies of proteases have been an important area of research of this Section since its establishment. We have been particularly active in the investigation of structure-function relationship in aspartic proteases, including clinically important retroviral enzymes. Our studies of HIV protease, although no longer a major target of active research, are still ongoing and concentrate on the investigation of drug-resistant variants and their complexes with inhibitors. We have investigated retroviral proteases from several other sources such as FIV, RSV, and HTLV-1. A number of inhibitor complexes of the latter enzyme have been analyzed, with the aim of assisting in the development of drugs against HTLV-caused leukemia. Cockroach allergen Bla g 2 was shown to be an inactive aspartic protease and we solved the structures of two complexes with different specific antibodies. We have established an extensive program of investigating serine-carboxyl peptidases (sedolisins), a family that was first characterized based on crystal structures solved in this laboratory and that is found in many different organisms. We are also investigating a bacterial ATP-dependent protease Lon, finding that is proteolytic domain has a unique fold and thus establishes a new family of proteases with a Ser-Lys catalytic dyad. Lectins with antiviral activity We have been involved in studies of several lectins with antiviral activities, some of them currently being in pre-clinical trials as potential drugs preventing HIV infection. We have solved the structure of griffithsin, as free protein and complexed with a number of mono- and disaccharides, explaining the structural basis for its tight binding to branched mannose-rich carbohydrates. We have reengineered griffithsin into a monomeric form and solved its structure with a complex oligosaccharide, elucidating the basis of its antiviral properties. We have also solved atomic-resolution structure of another lectin, scytovirin. Cytokines and cytokine receptors Our Section has been investigating the crystal structures of several cytokines and has made progress in preparing their receptor complexes. We have purified and crystallized complexes of IL-10 with its specific receptor and are studying complexes of several other cytokines related to IL-10, such as IL-19, IL-20, and IL-22. We have solved the structure of lambda interferon complexed with its receptor. Development of crystallographic methodology We have been investigating the problems related to phasing of diffraction data, deposition of structures in the Protein Data Bank, and improvement of the quality of deposited crystallographic data.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Investigator-Initiated Intramural Research Projects (ZIA)
Project #
1ZIABC010348-10
Application #
7965279
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
10
Fiscal Year
2009
Total Cost
$1,774,669
Indirect Cost
Name
National Cancer Institute Division of Basic Sciences
Department
Type
DUNS #
City
State
Country
Zip Code
Ottaiano, Tatiana F; Andrade, Sheila S; de Oliveira, Cleide et al. (2017) Plasma kallikrein enhances platelet aggregation response by subthreshold doses of ADP. Biochimie 135:72-81
Lubkowski, Jacek; Durbin, Sarah V; Silva, Mariana C C et al. (2017) Structural analysis and unique molecular recognition properties of a Bauhinia forficata lectin that inhibits cancer cell growth. FEBS J 284:429-450
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Jha, Jyoti K; Li, Mi; Ghirlando, Rodolfo et al. (2017) The DnaK Chaperone Uses Different Mechanisms To Promote and Inhibit Replication of Vibrio cholerae Chromosome 2. MBio 8:
Wlodawer, Alexander (2017) Stereochemistry and Validation of Macromolecular Structures. Methods Mol Biol 1607:595-610
Wlodawer, Alexander; Dauter, Zbigniew (2017) `Atomic resolution': a badly abused term in structural biology. Acta Crystallogr D Struct Biol 73:379-380
Wlodawer, Alexander (2017) Online tools for enhancing presentation, understanding, and retention of 3D structural data. FEBS J 284:3974-3976
Zhang, Di; Wlodawer, Alexander; Lubkowski, Jacek (2016) Crystal Structure of a Complex of the Intracellular Domain of Interferon ? Receptor 1 (IFNLR1) and the FERM/SH2 Domains of Human JAK1. J Mol Biol 428:4651-4668
Woodfolk, Judith A; Glesner, Jill; Wright, Paul W et al. (2016) Antigenic Determinants of the Bilobal Cockroach Allergen Bla g 2. J Biol Chem 291:2288-301
Dauter, Zbigniew; Wlodawer, Alexander (2016) Progress in protein crystallography. Protein Pept Lett 23:201-10

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