Abstract

Evidence has accumulated indicating that a highly conserved hydrophobic domain usually near the amino terminus of viral transmembrane proteins plays critical roles in the infection process. These viral fusion sequences insert into and destabilize the cell membrane and act in concert with the viral and cellular proteins and lipids to form a pore through which the viral nucleic acid can pass. Site-directed mutagenesis has shown that replacement of key residues in the influenza virus hemagglutinin (HA2) and the HIV glycoprotein 41 (gp41) fusion sequences can dramatically affect viral fusion. Synthetic """"""""fusion peptides"""""""" (FP) corresponding to the fusion sequences, induce lipid mixing and lysis with liposomes and cell membranes. Some studies with synthetic FP representing the mutated viral fusion sequences have better defined the structural origins of the altered viral fusion. However there is still limited information concerning the relationship of viral FP structure to their mechanism of action. This research proposal is based on the hypothesis that understanding of the role of the fusion sequence in virus-cell fusion can be enhanced by defining the detailed structural and functional changes brought about by replacement of key residues in synthetic fusion peptides. The objective is to determine the structural characteristics of viral FP that are necessary for fusion competence. Using FP based on mutated viral sequences, we will seek correlations between their altered activity and membrane bound structure. The influenza, HIV and variant FP will be tested for lytic and fusogenic activity with red blood cells and liposomes. The nature and extent of the FP and variant perturbation of membrane lipid will be investigated with 31P-NMR, polarized Fourier Transform Infrared (FTIR) and Electron Spin Resonance (ESR) spectroscopy. The conformation, orientation and topography of fusion peptides in membranes or membrane mimicking solvents will also be examined with Circular Dichroism (CD), FTIR, and ESR spectroscopy. FTIR of 13C-labeled peptides will be used to assess local conformations. Based on these structural studies, we will then construct molecular models for the interaction of each FP and variant with membrane lipids.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Minority Biomedical Research Support - MBRS (S06)
Project #
5S06GM053933-05
Application #
6458446
Study Section
Minority Programs Review Committee (MPRC)
Project Start
2001-06-01
Project End
2002-05-31
Budget Start
Budget End
Support Year
5
Fiscal Year
2001
Total Cost
Indirect Cost

  Institution

Name
California State Polytechnic University Pomona
Department
Type
DUNS #
City
Pomona
State
CA
Country
United States
Zip Code
91768

  Publications

Dadgar, Saedeh; Floriano, Wely B (2015) Systematic discovery of molecular probes targeting multiple non-orthosteric and spatially distinct sites in the botulinum neurotoxin subtype A (BoNT/A). Mol Cell Probes 29:135-43
Dadgar, Saedeh; Ramjan, Zack; Floriano, Wely B (2013) Paclitaxel is an inhibitor and its boron dipyrromethene derivative is a fluorescent recognition agent for botulinum neurotoxin subtype A. J Med Chem 56:2791-803
Chew, Tina W; Jiang, Xinyin; Yan, Jian et al. (2011) Folate intake, MTHFR genotype, and sex modulate choline metabolism in mice. J Nutr 141:1475-81
Liang, M T C; Braun, W; Bassin, S L et al. (2011) Effect of high-impact aerobics and strength training on BMD in young women aged 20-35 years. Int J Sports Med 32:100-8
Yan, Jian; Wang, Wei; Gregory 3rd, Jesse F et al. (2011) MTHFR C677T genotype influences the isotopic enrichment of one-carbon metabolites in folate-compromised men consuming d9-choline. Am J Clin Nutr 93:348-55
Shin, William; Yan, Jian; Abratte, Christian M et al. (2010) Choline intake exceeding current dietary recommendations preserves markers of cellular methylation in a genetic subgroup of folate-compromised men. J Nutr 140:975-80
Austin, Misa U; Liau, Wei-Siang; Balamurugan, Krishnaswamy et al. (2010) Knockout of the folate transporter folt-1 causes germline and somatic defects in C. elegans. BMC Dev Biol 10:46
Caudill, Marie A; Dellschaft, Neele; Solis, Claudia et al. (2009) Choline intake, plasma riboflavin, and the phosphatidylethanolamine N-methyltransferase G5465A genotype predict plasma homocysteine in folate-deplete Mexican-American men with the methylenetetrahydrofolate reductase 677TT genotype. J Nutr 139:727-33
Ivanov, Alexandre; Nash-Barboza, Susan; Hinkis, Sabrina et al. (2009) Genetic variants in phosphatidylethanolamine N-methyltransferase and methylenetetrahydrofolate dehydrogenase influence biomarkers of choline metabolism when folate intake is restricted. J Am Diet Assoc 109:313-8
Lee, Justine; Bernard, Steven; Liu, Xiao-Chuan (2009) Nanostructured Biomimetic Catalysts for Asymmetric Hydrogenation of Enamides using Molecular Imprinting Technology. React Funct Polym 69:650-654

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