Abstract

The central objective of this competing continuation research is to use structure-based mimetics to design antagonists for IL5 and to advance mechanistic understanding of receptor recognition for IL5 specific and for 4-helix bundle growth factor proteins generally. IL5 is the major hematopoietin which stimulates the proliferation, migration and activation of eosinophils and has been implicated in the pathogenesis of diseases such as asthma. Indeed, neutralizing IL5 antibodies currently are yielding promising results in asthma clinical trials, providing a proof of principle for the potential benefit of IL5 antagonists in therapies for asthma and other allergic diseases. IL5 is a homodimeric protein, dominated by two 4-helix bindle conformational domains. It functions through a cell-surface receptor that contains an alpha chain that binds IL5 selectively and a more 'public' beta chain for signal transduction. Available data for IL5 provide an important opportunity to use recognition site mimetics to decipher basic structural principles about how the 4-helix bundle framework in IL5 displays receptor binding epitopes for alpha and beta chains and to provide mimetic strategies useful to design 4-helix bundle cytokine antagonists. This project has several specific aims: (1) advance growing understanding of activating and non-activating modes of receptor subunit recruitment and design IL5 mimetic monomer and chimera antagonists, which recruit without activation; (2) starting with key miniprotein mimetic leads based on coiled coil stem loop scaffold, design advanced miniprotein antagonists, including size-minimized coiled-coil structures and miniproteins with alternative conformational scaffolds; (3) map and compare ligand binding epitopes on receptor alpha chain for IL5 vs. protein and miniprotein mimetic antagonists through mutational studies of the receptor and complementary mutagenesis of the ligands; (4) advance the use of mimetics through protein minimization, miniprotein scaffolds and antibody CDRs using the structurally related granulocyte- macrophage colony stimulating factor system. Long term, this project will lead to a fundamental understanding of recognition epitopes within the structural architecture of IL5. It will yield models for how variations within the basic 4-helix bundle architecture, common to many growth factor protein, trigger selective receptor recognition. And it will yield antagonist strategies which could lead to molecular tools for therapeutic intervention in asthma and other allergic diseases.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI040462-06
Application #
6497081
Study Section
Bio-Organic and Natural Products Chemistry Study Section (BNP)
Program Officer
Plaut, Marshall
Project Start
1996-12-01
Project End
2003-02-14
Budget Start
2002-02-01
Budget End
2003-02-14
Support Year
6
Fiscal Year
2002
Total Cost
$317,000
Indirect Cost

  Institution

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

  Publications

Ishino, Tetsuya; Economou, Nicoleta J; McFadden, Karyn et al. (2011) A protein engineering approach differentiates the functional importance of carbohydrate moieties of interleukin-5 receptor ýý. Biochemistry 50:7546-56
Zaks-Zilberman, Meirav; Harrington, Adrian E; Ishino, Tetsuya et al. (2008) Interleukin-5 receptor subunit oligomerization and rearrangement revealed by fluorescence resonance energy transfer imaging. J Biol Chem 283:13398-406
Ishino, Tetsuya; Harrington, Adrian E; Zaks-Zilberman, Meirav et al. (2008) Slow-dissociation effect of common signaling subunit beta c on IL5 and GM-CSF receptor assembly. Cytokine 42:179-90
Bhattacharya, Madhushree; Pillalamari, Udaya; Sarkhel, Sanjay et al. (2007) Recruitment pharmacophore for interleukin 5 receptor alpha antagonism. Biopolymers 88:83-93
Ishino, Tetsuya; Pillalamarri, Udaya; Panarello, Dominick et al. (2006) Asymmetric usage of antagonist charged residues drives interleukin-5 receptor recruitment but is insufficient for receptor activation. Biochemistry 45:1106-15
Ishino, Tetsuya; Robertson, Noreen; Chaiken, Irwin (2005) Cytokine recognition by human interleukin 5 receptor. Vitam Horm 71:321-44
Ishino, Tetsuya; Urbina, Cecilia; Bhattacharya, Madhushree et al. (2005) Receptor epitope usage by an interleukin-5 mimetic peptide. J Biol Chem 280:22951-61
Ishino, Tetsuya; Pasut, Gianfranco; Scibek, Jeffery et al. (2004) Kinetic interaction analysis of human interleukin 5 receptor alpha mutants reveals a unique binding topology and charge distribution for cytokine recognition. J Biol Chem 279:9547-56
Ruchala, Piotr; Varadi, Gyorgyi; Ishino, Tetsuya et al. (2004) Cyclic peptide interleukin 5 antagonists mimic CD turn recognition epitope for receptor alpha. Biopolymers 73:556-68
Li, Chuanzhao; Plugariu, Carmela G; Bajgier, Joanna et al. (2002) Coiled coil miniprotein randomization on phage leads to charge pattern mimicry of the receptor recognition determinant of interleukin 5. J Mol Recognit 15:33-43

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