Abstract

EXCEED THE SPACE PROVIDED. Exploration of a natural product's mode of action often sheds light on basic areas of biology not easily studied by traditional approaches. This bioorganic strategy to cell biology has led to significant advances in the study of immunoregulation using the natural products, FK506, cyclosporin, and rapamycin. In addition, the investigationof how potent biologically active natural products work at the molecular level (through the identification of their intracellular protein receptors), can lead to the identification of key proteins within a complex intracellular process. These natural product target proteins are, by definition, 'pharmaceutically vulnerable' and thus can serve as novel drug targets. This proposal focuses on the modes of action of two natural products; the anti-inflammatory fungal metabolite isopanepoxydone and the potent antitumor macrolide amphidinolide B isolated from an Okinawan dinoflagellate. Isopanepoxydone blocks the DNA binding activity of NF-KB, a key transcription factor that mediates pro-inflammatory signal-induced gene transcription. This is mediated via inhibition of 1KB degradation, a protein that negatively regulates the activity of NF-KB. Although much is known about the downstream consequences of isopanepoxydone's anti-inflammatoryaction, the protein target of this natural product that lies upstream of 1KBis unknown. Towards the goal of identifying the intracellular target of isopanepoxydone, we have modified our previously reported synthetic route to generate a biotinylated isopanepoxydone affinity reagent. Here, we present evidence for a 48kDa protein that covalently and specifically binds to this isopanepoxydone affinity reagent. The objective of this research is to understand the molecular mechanisms by which isopanepoxydone inhibits pro-inflammatory signal transduction through the purification, identification and characterization of this 48kDa isopanepoxydone binding protein. The anti-tumor macrolide amphidinolide B is at an earlier stage in the mode of action elucidation process. We propose here a novel retrosynthetic disconnection strategy for the total synthesis of this potent natural product. This synthetic effort will also afford the facile generation of a biotinylated affinity reagent, with which we plan to purify, identify and clone amphidinolide B binding proteins. Biochemical and cell biological characterizationof these amphidinolidebinding proteins will confirm their role in mediating the potent cytotoxicity of the natural product. We have successfully employed this same chemical/biochemical/cell biological approach to identify and characterize the intracellular receptors of the antiangiogenic natural product, rumagillin, the anti-inflammatory agent, parthenolide, and the antitumor compounds, epoxomicin and eponemycin. PERFORMANCE SITE ========================================Section End===========================================

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
3R01GM062120-07S1
Application #
7029316
Study Section
Bio-Organic and Natural Products Chemistry Study Section (BNP)
Program Officer
Lograsso, Philip
Project Start
2005-03-01
Project End
2005-07-31
Budget Start
2005-03-01
Budget End
2005-07-31
Support Year
7
Fiscal Year
2005
Total Cost
$89,925
Indirect Cost

  Institution

Name
Yale University
Department
Physiology
Type
Schools of Arts and Sciences
DUNS #
043207562
City
New Haven
State
CT
Country
United States
Zip Code
06520

  Publications

Kim, Kyung Bo; Crews, Craig M (2013) From epoxomicin to carfilzomib: chemistry, biology, and medical outcomes. Nat Prod Rep 30:600-4
Tae, Hyun Seop; Hines, John; Schneekloth, Ashley R et al. (2011) Unexpected stereochemical tolerance for the biological activity of tyroscherin. Bioorg Med Chem 19:1708-13
Tae, Hyun Seop; Hines, John; Schneekloth, Ashley R et al. (2010) Total synthesis and biological evaluation of tyroscherin. Org Lett 12:4308-11
Custar, Daniel W; Zabawa, Thomas P; Hines, John et al. (2009) Total synthesis and structure-activity investigation of the marine natural product neopeltolide. J Am Chem Soc 131:12406-14
Kim, Kyung Bo; Crews, Craig M (2008) Chemical genetics: exploring the role of the proteasome in cell biology using natural products and other small molecule proteasome inhibitors. J Med Chem 51:2600-5
Hines, John; Groll, Michael; Fahnestock, Margaret et al. (2008) Proteasome inhibition by fellutamide B induces nerve growth factor synthesis. Chem Biol 15:501-12
Corson, Timothy W; Crews, Craig M (2007) Molecular understanding and modern application of traditional medicines: triumphs and trials. Cell 130:769-74
Petri, Andreas F; Schneekloth Jr, John S; Mandal, Amit K et al. (2007) Synthesis of the C3-C18 fragment of amphidinolides G and H. Org Lett 9:3001-4
Hines, John; Roy, Myriam; Cheng, Hua et al. (2006) Myriaporone 3/4 structure--activity relationship studies define a pharmacophore targeting eukaryotic protein synthesis. Mol Biosyst 2:371-9
Schneekloth Jr, John S; Sanders, John L; Hines, John et al. (2006) Neurotrophic peptide aldehydes: solid phase synthesis of fellutamide B and a simplified analog. Bioorg Med Chem Lett 16:3855-8

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