Abstract

The present proposal will continue efforts in a comprehensive drug discovery group to develop HIV-1 receptor inhibitors. Such inhibitors will block the interaction of HIV-1 gp120 envelope protein with CD4 transmembrane molecule found on human T lymphocytes and monocytes. During the last funding period, human recombinant soluble CD4 molecules were produced, crystallized and the structure of the amino terminal two domains (sCD41-183) determined to 2 angstroms surface patch on the C'C"""""""" ridge of CD4 domain 1. Three sets of investigators will now exploit their collective talents in immunology structural biology and medicinal chemistry to identify lead compounds for this purpose. Project 1 will purify existing recombinant CHO-derived gp120 as well as engineer and produce baculovirus-derived gp120 from SF2 and other HIV-1 strains. In addition, truncation/deletion/glycosylation mutants of gp120 variants will be produced. These molecules will be individually complexed to sCD41-183, further purified and the complexes resolved crystallographically by the project 5. Once the structure of a single CD4-gp120 complex is determined, gp120 derived from a different strain will be selected as an additional source for complex formation and structural analysis. Comparison of CD4 binding pockets in gp120 from different viral sources will identify the common, strain-independent features of the CD4-gp120 interaction. The coordinates of the complexes will be exploited in Project 6 to generate a list of putative CD4 or gp120 binding compounds through DOCK computational methods. These will be tested for activity in a variety of directed molecular screens and HIV-1 replication assays. In addition, chemical analogs of existing, non-immunosuppressive DOCK-based organic leads (lesser than 1000 MW) will be synthesized, which were designed to bind to CD4 and are known to inhibit the HIV-1 gp120 CD4 interaction and HIV-1 viral replication at micromolar concentrations. Efforts to co-crystallize these compounds with CD4 are presently underway in Project 5 and will greatly aid the design task. Finally, direct chemical approaches to mimic the domain 1 C'C"""""""" turn as well as the C"""""""" strand will be assessed by NMR and functional studies. The non-immunosuppressive nature of potential lead compounds will be verified by functional assays in conjunction with detailed mapping studies of the class II MHC binding site on CD4.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project--Cooperative Agreements (U01)
Project #
5U01AI027336-09
Application #
2003502
Study Section
Special Emphasis Panel (SRC (47))
Project Start
1988-09-30
Project End
1998-09-30
Budget Start
1996-12-01
Budget End
1998-09-30
Support Year
9
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Dana-Farber Cancer Institute
Department
Type
DUNS #
149617367
City
Boston
State
MA
Country
United States
Zip Code
02215

  Publications

Ferrer, M; Harrison, S C (1999) Peptide ligands to human immunodeficiency virus type 1 gp120 identified from phage display libraries. J Virol 73:5795-802
Tan, K; Liu, J; Wang, J et al. (1997) Atomic structure of a thermostable subdomain of HIV-1 gp41. Proc Natl Acad Sci U S A 94:12303-8
Ferrer, M; Godbout, K L; Sullivan, B J et al. (1997) Construction and characterization of a radio-iodinatable mutant of recombinant human CD4. J Immunol Methods 210:215-25
Sakihama, T; Smolyar, A; Reinherz, E L (1995) Oligomerization of CD4 is required for stable binding to class II major histocompatibility complex proteins but not for interaction with human immunodeficiency virus gp120. Proc Natl Acad Sci U S A 92:6444-8
Sakihama, T; Smolyar, A; Reinherz, E L (1995) Molecular recognition of antigen involves lattice formation between CD4, MHC class II and TCR molecules. Immunol Today 16:581-7
Bell, K D; Ramilo, O; Vitetta, E S (1993) Combined use of an immunotoxin and cyclosporine to prevent both activated and quiescent peripheral blood T cells from producing type 1 human immunodeficiency virus. Proc Natl Acad Sci U S A 90:1411-5
Moebius, U; Pallai, P; Harrison, S C et al. (1993) Delineation of an extended surface contact area on human CD4 involved in class II major histocompatibility complex binding. Proc Natl Acad Sci U S A 90:8259-63
Moebius, U; Clayton, L K; Abraham, S et al. (1992) The human immunodeficiency virus gp120 binding site on CD4: delineation by quantitative equilibrium and kinetic binding studies of mutants in conjunction with a high-resolution CD4 atomic structure. J Exp Med 176:507-17
Moebius, U; Clayton, L K; Abraham, S et al. (1992) Human immunodeficiency virus gp120 binding C'C"" ridge of CD4 domain 1 is also involved in interaction with class II major histocompatibility complex molecules. Proc Natl Acad Sci U S A 89:12008-12
Ghetie, V; Wheeler, T; Scott, D et al. (1992) A CD4-derived peptide carrier blocks acute HIV-1 infection in vitro and binds to gp120 in the presence of Walter-Reed stage 1-6 HIV+ sera. AIDS Res Hum Retroviruses 8:1945-8

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