Abstract

The goal of this Proposal is to design, prepare, and analyze a variety of ligands as molecular probes in the study of protein-protein interactions between macromolecules involved in signal transduction. Specifically, these ligands will target selected members of the recently discovered PDZ domain family. PDZ domains have been identified in a number of different proteins that are involved in the assembly of receptors at cellular membranes, as well as proteins that participate in the formation of the extracellular matrix. While clearly playing a significant role in certain cellular processes, there is much that is not known about the in vivo consequences of PDZ domain- mediated interactions. From a biochemical point of view, there is a near-total absence of an understanding of the thermodynamics that governs the basic molecular recognition process involving PDZ domains. In the initial work of this Proposal, PDZ domains and binding peptide ligands will be studied using isothermal titration calorimetry (ITC), a powerful method that provides a thorough thermodynamic profile for binding (enthalpy, entropy, free energy, and dissociation constants). In addition, X-ray crystallographic structural determinations will be made of the PDZ-ligand complexes, allowing for a correlation of the thermodynamics of binding to specific molecular interactions. Novel ligands will then be designed based on this data, as well as existing structural information, with the ultimate goal of preparing cell-permeable, selective and potent PDZ domain binding ligands. These compounds could then be used in cellular studies and serve as molecular probes to decipher the biological functions of PDZ-mediated binding events. From a therapeutic perspective, recent reports demonstrate a strong link between certain PDZ-bearing proteins and oncogenic activity, and suggest that PDZ may represent a completely new target for anti-cancer drug design. The central focus, then, in this Proposal will be on two PDZ proteins that may reflect the fundamental binding preferences of all other PDZ domains: the Class I PDZ domains from PSD95, and the Class II PDZ domain from hCASK. An interdisciplinary approach towards characterizing PDZ domain binding will be conducted according to the following plan: (1) prepare PDZ proteins and peptide ligands, then study binding with ITC; (2) employ X-ray crystallography to evaluate the protein- bound conformations of the PDZ-binding ligands; (3) using structure-based and combinatorial chemistry methods, design and synthesize a variety of novel peptide analog ligands to identify binding probes with improved PDZ domain affinity and/or selectivity; and (4) devise supporting binding and cellular assays that will lead to more rapid evaluation of PDZ ligand affinity and the effects these compounds have on the biological function of cells that actively utilize PDZ-mediated interactions.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM063021-01A1
Application #
6435144
Study Section
Bio-Organic and Natural Products Chemistry Study Section (BNP)
Program Officer
Schwab, John M
Project Start
2002-03-01
Project End
2007-02-28
Budget Start
2002-03-01
Budget End
2003-02-28
Support Year
1
Fiscal Year
2002
Total Cost
$256,456
Indirect Cost

  Institution

Name
Wayne State University
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
City
Detroit
State
MI
Country
United States
Zip Code
48202

  Publications

Marshall, John; Wong, Kwoon Y; Rupasinghe, Chamila N et al. (2015) Inhibition of N-Methyl-D-aspartate-induced Retinal Neuronal Death by Polyarginine Peptides Is Linked to the Attenuation of Stress-induced Hyperpolarization of the Inner Mitochondrial Membrane Potential. J Biol Chem 290:22030-48
Muders, Michael H; Vohra, Pawan K; Dutta, Shamit K et al. (2009) Targeting GIPC/synectin in pancreatic cancer inhibits tumor growth. Clin Cancer Res 15:4095-103
Sharma, Sudhir C; Memic, Adnan; Rupasinghe, Chamila N et al. (2009) T7 phage display as a method of peptide ligand discovery for PDZ domain proteins. Biopolymers 92:183-93
Udugamasooriya, D Gomika; Sharma, Sudhir C; Spaller, Mark R (2008) A chemical library approach to organic-modified peptide ligands for PDZ domain proteins: a synthetic, thermodynamic and structural investigation. Chembiochem 9:1587-9
Memic, Adnan; Spaller, Mark R (2008) How do halogen substituents contribute to protein-binding interactions? A thermodynamic study of peptide ligands with diverse aryl halides. Chembiochem 9:2793-5
Saro, Dorina; Li, Tao; Rupasinghe, Chamila et al. (2007) A thermodynamic ligand binding study of the third PDZ domain (PDZ3) from the mammalian neuronal protein PSD-95. Biochemistry 46:6340-52
Klosi, Edvin; Saro, Dorina; Spaller, Mark R (2007) Bivalent peptides as PDZ domain ligands. Bioorg Med Chem Lett 17:6147-50
Sharma, Sudhir C; Rupasinghe, Chamila N; Parisien, Rachel B et al. (2007) Design, synthesis, and evaluation of linear and cyclic peptide ligands for PDZ10 of the multi-PDZ domain protein MUPP1. Biochemistry 46:12709-20
McAuliffe, P F; Murday, M E; Efron, P A et al. (2006) Dose-dependent improvements in outcome with adenoviral expression of interleukin-10 in a murine model of multisystem organ failure. Gene Ther 13:276-82
Udugamasooriya, Gomika; Saro, Dorina; Spaller, Mark R (2005) Bridged peptide macrocycles as ligands for PDZ domain proteins. Org Lett 7:1203-6

Showing the most recent 10 out of 13 publications