Abstract

This proposal describes the synthesis and studies of the ocimyquines and gukulenins, natural products that exhibit potent antimalarial and antiproliferative effects, respectively. Ocimyquines are nanomolar inhibitors of malaria parasites that are equally potent against drug-sensitive and -resistant strains, and have demonstrated high therapeutic indices in cell culture. In addition, they display prophylactic and curative activty in mouse models, without measurable toxicity. The gukulenins are low nanomolar inhibitors of several cancer cell lines and are very promising candidates for the treatment of colorectal cancer, the second-leading cause of cancer-related deaths in the United States. Both families of natural products possess molecular architectures that are unique. The ocimyquines contain a tetrasubstituted aminocyclopropane embedded within a pentacyclic carbon skeleton whereas the gukulenins are dimeric a-tropolone natural products containing six carbocyclic rings. Although these two families of compounds are unique among anti-infectives and anti-proliferative compounds, and show potent and potentially clinically-useful activities, no syntheses or synthetic studies have been reported. In addition, little is known about their structure-function relationships, and the mechanisms underlying their efficacy and selectivity remain unknown. The objectives of this proposal are to complete concise and convergent syntheses of the ocimyquines and gukulenins and evaluate their efficacy as radical cure anti-malarials and anti-proliferative agents. We have made significant progress toward the syntheses of both families of metabolites, having developed chemistry to access many of the key substructures of the targets. Our synthetic efforts have led to the development of new methods for the synthesis of tetrasubstituted aminocyclopropanes by a ring expansion-ring contraction strategy and 3,5,6-trisubsituted-a-tropolone rings by a novel reductive cleavage reaction. The collaborative nature of the proposal provides the infrastructure required to evaluate the antimalarial prophylactic and therapeutic activity of the ocimyquines and their synthetic derivatives and to elucidate their biological target. In addition, we will conduct structure-functin studies of the gukulenins, test the hypothesis that the natural products engage in reversible covalent bond formation with their target, and identify candidate binding proteins. These experiments will lead to the identification of new antimalarial and anticancer agents with improved potencies and activities, provide insights into the biological mechanisms underlying these activities, and lay the foundation for their preclinical evaluation as new treatments for malaria and colorectal cancer.

Public Health Relevance

The development of new medicines for the treatment of human diseases is central to the mission of the National Institutes of Health. This proposal focuses on the synthesis and evaluation of new natural product-derived anticancer and antimalarial agents. This work build upon the well-established ethnobotanical history of efficacy and safety of some of the natural products described in this proposal as well as preliminary evidence of their potency and selectivity.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM110506-02
Application #
9140068
Study Section
Synthetic and Biological Chemistry B Study Section (SBCB)
Program Officer
Lees, Robert G
Project Start
2015-09-08
Project End
2019-05-31
Budget Start
2016-06-01
Budget End
2017-05-31
Support Year
2
Fiscal Year
2016
Total Cost
Indirect Cost

  Institution

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

  Publications

Thekkiniath, Jose; Mootien, Sara; Lawres, Lauren et al. (2018) BmGPAC, an Antigen Capture Assay for Detection of Active Babesia microti Infection. J Clin Microbiol 56:
Tripathi, Prabhanshu; Shine, Emilee E; Healy, Alan R et al. (2017) ClbS Is a Cyclopropane Hydrolase That Confers Colibactin Resistance. J Am Chem Soc 139:17719-17722
Trautman, Eric P; Healy, Alan R; Shine, Emilee E et al. (2017) Domain-Targeted Metabolomics Delineates the Heterocycle Assembly Steps of Colibactin Biosynthesis. J Am Chem Soc 139:4195-4201
Murphy, Stephen K; Zeng, Mingshuo; Herzon, Seth B (2017) A modular and enantioselective synthesis of the pleuromutilin antibiotics. Science 356:956-959
Nikolayevskiy, Herman; Moe Tun, Maung Kyaw; Rablen, Paul R et al. (2017) A complex stereochemical relay approach to the antimalarial alkaloid ocimicide A1. Evidence for a structural revision. Chem Sci 8:4867-4871
Zeng, Mingshuo; Murphy, Stephen K; Herzon, Seth B (2017) Development of a Modular Synthetic Route to (+)-Pleuromutilin, (+)-12-epi-Mutilins, and Related Structures. J Am Chem Soc 139:16377-16388
Guntaka, Naga Sandhya; Healy, Alan R; Crawford, Jason M et al. (2017) Structure and Functional Analysis of ClbQ, an Unusual Intermediate-Releasing Thioesterase from the Colibactin Biosynthetic Pathway. ACS Chem Biol 12:2598-2608
Healy, Alan R; Vizcaino, Maria I; Crawford, Jason M et al. (2016) Convergent and Modular Synthesis of Candidate Precolibactins. Structural Revision of Precolibactin A. J Am Chem Soc 138:5426-32
Healy, Alan R; Nikolayevskiy, Herman; Patel, Jaymin R et al. (2016) A Mechanistic Model for Colibactin-Induced Genotoxicity. J Am Chem Soc 138:15563-15570
Hart, Robert J; Cornillot, Emmanuel; Abraham, Amanah et al. (2016) Genetic Characterization of Plasmodium Putative Pantothenate Kinase Genes Reveals Their Essential Role in Malaria Parasite Transmission to the Mosquito. Sci Rep 6:33518

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