Abstract

During the past year, this laboratory continued studies on the mechanism of HIV entry, and on the development of novel protective and treatment strategies based on the molecules involved in entry. 1) Molecular mechanisms of HIV Env-mediated entry/fusion. a) Effects of synthetic peptides based on the extracellular loop of CCR5 on Env function. We found that peptides from each of the extracellular loops inhibited fusion and infection mediated by CCR5-using Envs, but not by Envs that cannot use CCR5. Several lines of evidence indicated that the peptides act by binding to Env. b) Design of a soluble CCR5 mimic. We have initiated collaborative efforts to design a soluble protein containing the extracellular loops of CCR5, with the hope that it will bind to the CCR5-binding region of gp120. 2) Novel anti-HIV agents based on HIV Env/receptor interactions. a) sCD4-17b, a potent HIV-1 neutralizing agent. sCD4-17b is a recombinant chimeric protein containing soluble CD4 attached via a long flexible polypeptide linker to a single chain antibody that binds to a CD4-induced epitope of gp120 involved in binding to coreceptor. While the protein neutralizes some HIV-1 strains with extremely high potency, other strains appear resistant, despite the known presence of binding sites for CD4 and 17b. We hypothesize that the resistance of these isolates reflects structural features of the corresponding gp120 molecules (V1/V2 and V3 loops, glycosylation) that renders the original linker (35 residues) insufficiently long to enable simultaneous binding of the CD4 and 17b moieties. We have engineered sCD4-17b variants with longer linker lengths, and prepared corresponding recombinant baculoviruses for high level expression. We have also continued efforts to express sCD4-17b in Lactobacillus, with the idea of colonizing the vaginal tract to provide a means for protection against sexual transmission that is durable, economically feasible, and controlled by women. b) Anti-HIV immunotoxin. NIH has licensed 3B3-PE38 to IVAX, to produce clinical grade material for Phase I trials. We have also initiated a collaboration to test the efficacy of anti-HIV immunotoxins in SHIV-infected rhesus macaques.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Intramural Research (Z01)
Project #
1Z01AI000538-16
Application #
6808245
Study Section
(LVD)
Project Start
Project End
Budget Start
Budget End
Support Year
16
Fiscal Year
2003
Total Cost
Indirect Cost

  Institution

Name
Niaid Extramural Activities
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Salzwedel, Karl; Berger, Edward A (2009) Complementation of diverse HIV-1 Env defects through cooperative subunit interactions: a general property of the functional trimer. Retrovirology 6:75
Berger, Edward A; Alkhatib, Ghalib (2007) HIV gp120 interactions with coreceptors: insights from studies with CCR5-based peptides. Eur J Med Res 12:403-7
Alkhatib, Ghalib; Berger, Edward A (2007) HIV coreceptors: from discovery and designation to new paradigms and promise. Eur J Med Res 12:375-84
Lusso, Paolo; Earl, Patricia L; Sironi, Francesca et al. (2005) Cryptic nature of a conserved, CD4-inducible V3 loop neutralization epitope in the native envelope glycoprotein oligomer of CCR5-restricted, but not CXCR4-using, primary human immunodeficiency virus type 1 strains. J Virol 79:6957-68
Lagenaur, Laurel A; Berger, Edward A (2005) An anti-HIV microbicide comes alive. Proc Natl Acad Sci U S A 102:12294-5
Agrawal, Lokesh; VanHorn-Ali, Zainab; Berger, Edward A et al. (2004) Specific inhibition of HIV-1 coreceptor activity by synthetic peptides corresponding to the predicted extracellular loops of CCR5. Blood 103:1211-7
Dey, Barna; Del Castillo, Christie S; Berger, Edward A (2003) Neutralization of human immunodeficiency virus type 1 by sCD4-17b, a single-chain chimeric protein, based on sequential interaction of gp120 with CD4 and coreceptor. J Virol 77:2859-65
Farber, Joshua M; Berger, Edward A (2002) HIV's response to a CCR5 inhibitor: I'd rather tighten than switch! Proc Natl Acad Sci U S A 99:1749-51
McHugh, Louise; Hu, Stella; Lee, B K et al. (2002) Increased affinity and stability of an anti-HIV-1 envelope immunotoxin by structure-based mutagenesis. J Biol Chem 277:34383-90
Schito, M L; Kennedy, P E; Kowal, R P et al. (2001) A human immunodeficiency virus-transgenic mouse model for assessing interventions that block microbial-induced proviral expression. J Infect Dis 183:1592-600

Showing the most recent 10 out of 17 publications