Abstract

The central objective of this Project is to use miniprotein mimetics together with the structure of the gp120KD4 complex to design antagonists of the interaction of HIV-1 with human cells. T-cell docking and entry by HIV-1, a major route of cell infection in AIDS, is driven by specific recognition of T-cell surface protein CD4 and chemokine coreceptor by HIV envelope protein gp120. The crystallographic structure of CD4 is known, as is its complex with gp120 and the coreceptor surrogate antibody 17b. The structural nature and interrelationship of gp 120 binding sites for CD4 and coreceptor have been revealed. The advancing high-resolution structural understanding of the protein participants in virus-cell recognition, together with the advancing technology of mimetics design, now make it possible to use miniprotein engineering coordinately with biophysical and biologicalanalysis to obtain an advanced mechanistic understanding of the structural basis of the CD4-gp120interaction process. This mechanistic understanding will help guide the design of new antagonists for HIV infection.
The specific aims are: (1) Construct novel miniprotein mimetics of CD4 using synthetic and complementary phage randomization methodologies and optimize their affinities for HIV- 1 envelope; (2) Identify key structural elements in miniprotein mimetics of CD4 that control activation of the coreceptor binding site of HIV-1 Env, and form miniprotein variants which favor Env binding with diminished coreceptor site activation; (3) Determine structural and interaction properties of miniprotein mimetics with trimeric vs monomeric forms of HIV- 1 envelopes, including ectodomain and membrane-associated forms, and refine the topological map of key structural elements needed for HIV-1-cell attachment and attachment antagonists. Overall, this project will yield an advanced definition of key structural elements at the interface of the CD4-gp 120 complex that trigger increased HIV- 1 envelope affinity for co-receptor and consequent cell infection; improved understanding of the CD4-viral envelope-coreceptor molecular machine that drives HIV- 1 attachment and infection of host cells; and molecular leads for new antagonist candidates for antiviral therapy. The miniprotein mimetics strategies derived will be useful to determine the mechanism of, and design antagonists for, other protein-protein interactions, such as the gp41 -gp 120 and chemokine receptor.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Program Projects (P01)
Project #
7P01GM056550-07
Application #
6800728
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
7
Fiscal Year
2002
Total Cost
$157,210
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Type
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Castillo-Menendez, Luis R; Witt, Kristen; Espy, Nicole et al. (2018) Comparison of Uncleaved and Mature Human Immunodeficiency Virus Membrane Envelope Glycoprotein Trimers. J Virol 92:
Rashad, Adel A; Song, Li-Rui; Holmes, Andrew P et al. (2018) Bifunctional Chimera That Coordinately Targets Human Immunodeficiency Virus 1 Envelope gp120 and the Host-Cell CCR5 Coreceptor at the Virus-Cell Interface. J Med Chem 61:5020-5033
Moraca, Francesca; Rinaldo, David; Smith 3rd, Amos B et al. (2018) Specific Noncovalent Interactions Determine Optimal Structure of a Buried Ligand Moiety: QM/MM and Pure QM Modeling of Complexes of the Small-Molecule CD4 Mimetics and HIV-1 gp120. ChemMedChem 13:627-633
Castillo-Menendez, Luis R; Nguyen, Hanh T; Sodroski, Joseph (2018) Conformational Differences Between Functional Human Immunodeficiency Virus (HIV-1) Envelope Glycoprotein Trimers and Stabilized Soluble Trimers. J Virol :
Madani, Navid; Princiotto, Amy M; Mach, Linh et al. (2018) A CD4-mimetic compound enhances vaccine efficacy against stringent immunodeficiency virus challenge. Nat Commun 9:2363
Kisalu, Neville K; Idris, Azza H; Weidle, Connor et al. (2018) A human monoclonal antibody prevents malaria infection by targeting a new site of vulnerability on the parasite. Nat Med 24:408-416
Parajuli, Bibek; Acharya, Kriti; Bach, Harry C et al. (2018) Restricted HIV-1 Env glycan engagement by lectin-reengineered DAVEI protein chimera is sufficient for lytic inactivation of the virus. Biochem J 475:931-957
Ma, Xiaochu; Lu, Maolin; Gorman, Jason et al. (2018) HIV-1 Env trimer opens through an asymmetric intermediate in which individual protomers adopt distinct conformations. Elife 7:
Johnson, Jacklyn; Zhai, Yinjie; Salimi, Hamid et al. (2017) Induction of a Tier-1-Like Phenotype in Diverse Tier-2 Isolates by Agents That Guide HIV-1 Env to Perturbation-Sensitive, Nonnative States. J Virol 91:
Herschhorn, Alon; Sodroski, Joseph (2017) An entry-competent intermediate state of the HIV-1 envelope glycoproteins. Receptors Clin Investig 4:

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