Abstract

The Structure Core will support all three projects in this U19. The goal of our U19 research program is to use structure-based rational design to combat influenza virus from both the therapeutic antibody and vaccine perspective. These endeavors, targeting the receptor-binding site (RBS) on hemagglutinin (HA), require many rounds of design and experimental validation executed in an iterative manner. Thus, the focus of this Core is three-fold: (i) Naturally occurring antibodies from Project 1 will be studied in complex with natural HA molecules. (ii) to solve structures of HA in complex with engineered antibodies from Project 2 for therapeutic applications, and (iii) to solve structures of HA engineered scaffolds in complex with known broadly neutralizing antibodies (bnAbs) in Project 3 for vaccine applications. We will use both electron microscopy (EM) and x-ray crystallography to accomplish these aims and generate sufficient structural coverage to enable development of anti-influenza solutions. Specifically, we will use electron microscopy (EM) to solve structures of HA in complex with engineered antibodies. EM is uniquely suited to rapidly generate structural information of protein complexes in a high-throughput manner. The information from EM can directly inform further structural and design efforts. We will employ both negative stain and cryo-EM methods to evaluate antibody-HA complexes at moderate and high resolution, respectively. We will also use x-ray crystallography to solve structures of HA and engineered HA scaffolds with antibodies. X-ray crystallography is routinely used to reveal atomic-level details of proteins and their complexes. Using the crystal screening capacity of The Joint Center for Structural Genomics housed at Scripps (Dr. Wilson is the PI), we can screen large numbers of antibodies, antigens, and conjugate complexes. We will use this pipeline to solve atomic-resolution structures of antibody-HA and antibody-scaffold complexes.

Public Health Relevance

This U19 focuses on designing novel antibodies and vaccine antigens for influenza. The structure of naturally occurring antibodies and antigens from Project 1 we will determined and passed on to Research Projects 2 and 3 for design purposes. Then, the structure of engineered antibodies and vaccines from Research Projects 2 and 3 will be determined to validate the models.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program--Cooperative Agreements (U19)
Project #
5U19AI117905-04
Application #
9475157
Study Section
Special Emphasis Panel (ZAI1)
Project Start
Project End
Budget Start
2018-05-01
Budget End
2019-04-30
Support Year
4
Fiscal Year
2018
Total Cost
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Type
DUNS #
079917897
City
Nashville
State
TN
Country
United States
Zip Code
37232

  Publications

Crowe Jr, James E (2018) Is It Possible to Develop a ""Universal"" Influenza Virus Vaccine? Potential for a Universal Influenza Vaccine. Cold Spring Harb Perspect Biol 10:
Bangaru, Sandhya; Zhang, Heng; Gilchuk, Iuliia M et al. (2018) A multifunctional human monoclonal neutralizing antibody that targets a unique conserved epitope on influenza HA. Nat Commun 9:2669
Wijesinghe, Kaveesha J; Urata, Sarah; Bhattarai, Nisha et al. (2017) Detection of lipid-induced structural changes of the Marburg virus matrix protein VP40 using hydrogen/deuterium exchange-mass spectrometry. J Biol Chem 292:6108-6122
Crowe Jr, James E (2017) Principles of Broad and Potent Antiviral Human Antibodies: Insights for Vaccine Design. Cell Host Microbe 22:193-206
Bruhn, Jessica F; Kirchdoerfer, Robert N; Urata, Sarah M et al. (2017) Crystal Structure of the Marburg Virus VP35 Oligomerization Domain. J Virol 91:
Chandra, Vikas; Wu, Dalei; Li, Sheng et al. (2017) The quaternary architecture of RAR?-RXR? heterodimer facilitates domain-domain signal transmission. Nat Commun 8:868
Sangha, Amandeep K; Dong, Jinhui; Williamson, Lauren et al. (2017) Role of Non-local Interactions between CDR Loops in Binding Affinity of MR78 Antibody to Marburg Virus Glycoprotein. Structure 25:1820-1828.e2
Labonte, Jason W; Adolf-Bryfogle, Jared; Schief, William R et al. (2017) Residue-centric modeling and design of saccharide and glycoconjugate structures. J Comput Chem 38:276-287
Tseng, Roger; Goularte, Nicolette F; Chavan, Archana et al. (2017) Structural basis of the day-night transition in a bacterial circadian clock. Science 355:1174-1180
Mousa, Jarrod J; Sauer, Marion F; Sevy, Alexander M et al. (2016) Structural basis for nonneutralizing antibody competition at antigenic site II of the respiratory syncytial virus fusion protein. Proc Natl Acad Sci U S A 113:E6849-E6858

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