Abstract

Heparanase is recognized as a master regulator of the aggressive phenotype of cancer, an important contributor to the poor outcome of cancer patients and a prime target for therapy. Although carbohydrate-based heparanase have been developed, but none were translated into use in the clinic. Additionally, interaction of heparanase with heparan sulfate (HS) is regulated by substrate sulfation sequences, and only substrates with specific sulfation patterns are cleaved by heparanase. Although the crystal structure of human heparanase has been recently resolved, it still does not allow determination of the structure of binding epitopes with defined N-and O- sulfation patterns at each subsite of heparanase. To address these challenges, Aim 1 entails a new modular chemical approach for the parallel combinatorial synthesis of a library of HS trisaccharide substrates, representing all possible N-acetyl as well as O- and N-sulfation motifs. Our strategy provides a systematic understanding of substrate specificity for heparanase and how heparanase selects favorable cleavage site.
In Aim 2, we propose to develop heparanase- inhibiting sulfated oligosaccharides of high efficacy and clinical applicability.
In Aim 3, the most potent inhibitors developed in Aim 2 will be tested for cross-bioactivity to other HS-binding proteins, which are responsible for mediating anticoagulant and angiogenic activity, antibody- induced thrombocytopenia, and tumor cell metastasis. With the ultimate goal of understanding if the in vitro inhibition of heparanase would translate in vivo, we will evaluate the effectiveness of the most potent inhibitor(s) in inhibiting lymphoma tumor growth and experimental metastasis. Together, this project will provide insight into sulfate-recognition motifs and favorable cleavage site for use to develop inhibitors of heparanase. The significant impact of this project is that, if successful, it could lead to the discovery of a heparanase-inhibiting small carbohydrate molecule for treatment of lymphomas, which are the fifth leading cancer in the North America, produce tumors predominantly in lymphoid structures.

Public Health Relevance

Heparanase is recognized as a master regulator of the aggressive phenotype of cancer, an important contributor to the poor outcome of cancer patients and a prime target for therapy. Although carbohydrate-based heparanase have been developed, but none were translated into use in the clinic. The goal of the proposal is to combine organic chemistry and tumor biology for the development of heparanase-inhibiting sulfated oligosaccharides of high efficacy and clinical applicability that could lead to the discovery of anti-cancer drug for treatment of lymphomas, the fifth leading cancer in the North America.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM098285-06A1
Application #
9816301
Study Section
Synthetic and Biological Chemistry A Study Section (SBCA)
Program Officer
Bond, Michelle Rueffer
Project Start
2012-04-01
Project End
2023-05-31
Budget Start
2019-09-01
Budget End
2020-05-31
Support Year
6
Fiscal Year
2019
Total Cost
Indirect Cost

  Institution

Name
Wayne State University
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
001962224
City
Detroit
State
MI
Country
United States
Zip Code
48202

  Publications

Sletten, Eric T; Loka, Ravi S; Yu, Fei et al. (2017) Glycosidase Inhibition by Multivalent Presentation of Heparan Sulfate Saccharides on Bottlebrush Polymers. Biomacromolecules 18:3387-3399
Loka, Ravi S; Yu, Fei; Sletten, Eric T et al. (2017) Design, synthesis, and evaluation of heparan sulfate mimicking glycopolymers for inhibiting heparanase activity. Chem Commun (Camb) 53:9163-9166
Sletten, Eric T; Ramadugu, Sai Kumar; Nguyen, Hien M (2016) Utilization of bench-stable and readily available nickel(II) triflate for access to 1,2-cis-2-aminoglycosides. Carbohydr Res 435:195-207
Yu, Fei; McConnell, Matthew S; Nguyen, Hien M (2015) Scalable synthesis of Fmoc-protected GalNAc-threonine amino acid and T(N) antigen via nickel catalysis. Org Lett 17:2018-21
Loka, Ravi S; McConnell, Matthew S; Nguyen, Hien M (2015) Studies of Highly-Ordered Heterodiantennary Mannose/Glucose-Functionalized Polymers and Concanavalin A Protein Interactions Using Isothermal Titration Calorimetry. Biomacromolecules 16:4013-4021
Sletten, Eric T; Svec, Riley L; Nguyen, Hien M (2015) Synthesis of a polymerizable, bivalent glycan mimetic of the HIV envelope spike gp120. Tetrahedron Lett 56:3473-3476
McKay, Matthew J; Park, Nathaniel H; Nguyen, Hien M (2014) Investigations of scope and mechanism of nickel-catalyzed transformations of glycosyl trichloroacetimidates to glycosyl trichloroacetamides and subsequent, atom-economical, one-step conversion to ?-urea-glycosides. Chemistry 20:8691-701
McKay, Matthew J; Nguyen, Hien M (2012) Recent Advances in Transition Metal-Catalyzed Glycosylation. ACS Catal 2:1563-1595
Yu, Fei; Nguyen, Hien M (2012) Studies on the selectivity between nickel-catalyzed 1,2-cis-2-amino glycosylation of hydroxyl groups of thioglycoside acceptors with C2-substituted benzylidene N-phenyl trifluoroacetimidates and intermolecular aglycon transfer of the sulfide group. J Org Chem 77:7330-43