Abstract

: Chemical processes that enable fragment union between complex coupling partners define a subset of reactions that are exceptionally powerful. While they can help to define efficient pathways to complex molecules, they are also of central importance to combinatorial and medicinal chemistry. Despite the importance of such coupling reactions in chemical synthesis, it is surprising that only a handful of robust pathways are available for bimolecular C-C bond formation between highly functionalized coupling partners. The research program outlined in this proposal is focused on establishing a new approach to stereoselective chemical synthesis that derives from discovery and application of novel metallacycle-mediated bimolecular C- C bond forming reactions in natural product synthesis. Our first phase of funding for GM080266 was focused on methods development, and a great many reactions have been discovered/reported over the last five years. We are now in a position to develop these unique modes of reactivity in the context of target-oriented synthesis. This is a critical component of the scientific advance we aim to make, as reaction methods need to be vetted in complex settings to explore their true potential in impacting medicinally relevant pursuits. As such, we will pursue the application of our technology to the syntheses of a range of structurally diverse and rare natural products (alkaloids, fatty acids and polyketides) that are known to possess significant and medicinally relevant biological activities. Overall, the program proposed will result in: (1) confirming the utility of metallacycle-mediated cross- coupling technology in complex molecule synthesis, (2) the elucidation of a range of novel retrosynthetic strategies in target-oriented synthesis, and (3) the first, or the most concise, syntheses of a range of natural products including, the alkaloid 205B, ripostatin A, borrelidin and kendomycin. Therefore, our proposed studies will aim to advance the emerging modes of chemical reactivity supported by GM080266 from a foundation of reaction methodology to a powerful class of stereoselective fragment coupling reactions of profound utility in target-oriented synthesis. As such, successful development of this program will offer advances in stereoselective synthesis that have great potential to impact the search for medicinally relevant small molecules via enabling future scientific discovery at the interface of chemistry with biology and medicine. II.

Public Health Relevance

: The manner in which complex molecules are synthesized greatly affects the role that organic chemistry plays in biology and medicine - a relationship that derives from the impact that chemical synthesis has on the availability of unique small molecules with medicinally relevant profiles. Chemical reactions that enable convergent coupling of complex partners are of central significance to organic synthesis, as they provide a means to both enhance efficiency in routes to intricate targets, and define workable schemes to establish SAR in medicinal chemistry. Described in this proposal is a scientific pursuit aimed at addressing the hypothesis that recently discovered fragment coupling reactions will have a profound and beneficial impact on the efficiency with which complex molecules are prepared - as evidenced by demonstrations in the context of rare natural products known to possess potent anticancer, antifungal, and antibiotic properties.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM080266-08
Application #
8535780
Study Section
Synthetic and Biological Chemistry B Study Section (SBCB)
Program Officer
Lees, Robert G
Project Start
2007-03-12
Project End
2013-05-31
Budget Start
2013-05-01
Budget End
2013-05-31
Support Year
8
Fiscal Year
2013
Total Cost
$65,311
Indirect Cost
$39,541

  Institution

Name
Scripps Florida
Department
Type
DUNS #
148230662
City
Jupiter
State
FL
Country
United States
Zip Code
33458

  Publications

Kim, Wan Shin; Du, Kang; Eastman, Alan et al. (2018) Synthetic nat- or ent-steroids in as few as five chemical steps from epichlorohydrin. Nat Chem 10:70-77
Micalizio, Glenn C; Mizoguchi, Haruki (2017) The Development of Alkoxide-Directed Metallacycle-Mediated Annulative Cross-Coupling Chemistry. Isr J Chem 57:228-238
Kier, Matthew J; Leon, Robert M; O'Rourke, Natasha F et al. (2017) Synthesis of Highly Oxygenated Carbocycles by Stereoselective Coupling of Alkynes to 1,3- and 1,4-Dicarbonyl Systems. J Am Chem Soc 139:12374-12377
O'Rourke, Natasha F; A, Mu; Higgs, Henry N et al. (2017) Function-Oriented Studies Targeting Pectenotoxin 2: Synthesis of the GH-Ring System and a Structurally Simplified Macrolactone. Org Lett 19:5154-5157
Aquino, Claudio; Greszler, Stephen N; Micalizio, Glenn C (2016) Synthesis of the Cortistatin Pentacyclic Core by Alkoxide-Directed Metallacycle-Mediated Annulative Cross-Coupling. Org Lett 18:2624-7
Cassidy, James S; Mizoguchi, Haruki; Micalizio, Glenn C (2016) Acceleration of metallacycle-mediated alkyne-alkyne cross-coupling with TMSCl. Tetrahedron Lett 57:3848-3850
Mizoguchi, Haruki; Micalizio, Glenn C (2016) Synthesis of Angularly Substituted trans-Fused Decalins through a Metallacycle-Mediated Annulative Cross-Coupling Cascade. Angew Chem Int Ed Engl 55:13099-13103
O'Rourke, Natasha F; Micalizio, Glenn C (2016) Cyclopropenes in Metallacycle-Mediated Cross-Coupling with Alkynes: Convergent Synthesis of Highly Substituted Vinylcyclopropanes. Org Lett 18:1250-3
Cheng, Xiayun; Micalizio, Glenn C (2016) Synthesis of Neurotrophic Seco-prezizaane Sesquiterpenes (1R,10S)-2-Oxo-3,4-dehydroneomajucin, (2S)-Hydroxy-3,4-dehydroneomajucin, and (-)-Jiadifenin. J Am Chem Soc 138:1150-3
O'Rourke, Natasha F; Kier, Matthew J; Micalizio, Glenn C (2016) Metallacycle-Mediated Cross-Coupling in Natural Product Synthesis. Tetrahedron 72:7093-7123

Showing the most recent 10 out of 46 publications