Abstract

Human parainfluenza virus type 3 (HPF3) is an important agent of lower respiratory tract disease in children. There are currently no treatments or vaccines available to combat this pediatric pathogen. Our studies have led to understanding of crucial factors controlling virus-host cell interactions for HPF3. The overall goal of the current proposal is to expand our investigation of the molecular pathogenesis of HPF3. The proposal integrates within in its aims the contributions of the virus and the host by focusing on mechanisms whereby the hemagglutinin-neuraminidase (HN) molecule carries out its roles in the viral life cycle and in pathogenesis in the lung. Our central hypothesis is that the interaction of HN with cellular receptor is critical for several essential components of the viral life cycle - entry, fusion and release - and that this interaction regulates pathogenicity. The specific objectives of the proposal are:(1) To investigate HN-receptor interaction in HPF3 fusion and entry. (A) We will evaluate whether the quantitative relationship between HN's receptor-binding and receptor-destroying functions determines the outcome of infection. The studies are an outgrowth of our demonstration that progeny virion release depends on the balance between HN's receptor binding affinity and neuraminidase activity. (B) We will identify how HN-receptor interaction contributes to triggering the fusion protein (F) to mediate fusion. This section evolves from our demonstration that HN receptor binding is the critical first step towards HN's role in fusion promotion and that HN activates F to fuse. (2) To analyze the role of HN in pathoqenesis of HPF3 in vivo using the cotton rat model. The studies follow from our demonstration that mutations in HN that alter HN-receptor interaction (but not replication) enhance pathogenesis in the cotton rat lung. We will ask whether: (A) it is the affinity of HN-receptor interaction or HN's fusion promotion activity that is a major determinant of virulence/pathogenesis in the lung; (B) the neuraminidase of HN determines the outcome of infection in the lung as it does in cell culture; (C) 4-GU-DANA (Zanamivir), which inhibits HN-receptor binding, alters the outcome of infection in the lung as it does in cell culture; and (D) viral resistance to 4-GU-DANA in vitro translates into 4-GU-DANA resistance in vivo. The proposed studies will lend insight into important molecular events in the life cycle of HPF3 and its interaction with the host, and will assist in the design of prevention and therapy.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI031971-16
Application #
7156961
Study Section
Experimental Virology Study Section (EVR)
Program Officer
Kim, Sonnie
Project Start
1992-04-01
Project End
2008-06-30
Budget Start
2007-01-01
Budget End
2008-06-30
Support Year
16
Fiscal Year
2007
Total Cost
$361,613
Indirect Cost

  Institution

Name
Weill Medical College of Cornell University
Department
Pediatrics
Type
Schools of Medicine
DUNS #
060217502
City
New York
State
NY
Country
United States
Zip Code
10065

  Publications

Iketani, Sho; Shean, Ryan C; Ferren, Marion et al. (2018) Viral Entry Properties Required for Fitness in Humans Are Lost through Rapid Genomic Change during Viral Isolation. MBio 9:
Mathieu, Cyrille; Porotto, Matteo; Figueira, Tiago N et al. (2018) Fusion Inhibitory Lipopeptides Engineered for Prophylaxis of Nipah Virus in Primates. J Infect Dis 218:218-227
Figueira, T N; Palermo, L M; Veiga, A S et al. (2017) In Vivo Efficacy of Measles Virus Fusion Protein-Derived Peptides Is Modulated by the Properties of Self-Assembly and Membrane Residence. J Virol 91:
Chen, Ya-Wen; Huang, Sarah Xuelian; de Carvalho, Ana Luisa Rodrigues Toste et al. (2017) A three-dimensional model of human lung development and disease from pluripotent stem cells. Nat Cell Biol 19:542-549
Figueira, Tiago N; Freire, João M; Cunha-Santos, Catarina et al. (2017) Quantitative analysis of molecular partition towards lipid membranes using surface plasmon resonance. Sci Rep 7:45647
Augusto, Marcelo T; Hollmann, Axel; Porotto, Matteo et al. (2017) Antiviral Lipopeptide-Cell Membrane Interaction Is Influenced by PEG Linker Length. Molecules 22:
Mathieu, Cyrille; Augusto, Marcelo T; Niewiesk, Stefan et al. (2017) Broad spectrum antiviral activity for paramyxoviruses is modulated by biophysical properties of fusion inhibitory peptides. Sci Rep 7:43610
Palermo, Laura M; Uppal, Manik; Skrabanek, Lucy et al. (2016) Features of Circulating Parainfluenza Virus Required for Growth in Human Airway. MBio 7:e00235
Mathieu, C; Huey, D; Jurgens, E et al. (2015) Prevention of measles virus infection by intranasal delivery of fusion inhibitor peptides. J Virol 89:1143-55
Gui, Long; Jurgens, Eric M; Ebner, Jamie L et al. (2015) Electron tomography imaging of surface glycoproteins on human parainfluenza virus 3: association of receptor binding and fusion proteins before receptor engagement. MBio 6:e02393-14

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