Abstract

This research program (CA-19033), now in the twenty-eighth year, embodies our long-term commitment to the complete structural characterization and efficient, enantioselective synthesis of architecturally challenging anticancer agents. The principle goals for the 29-31 years can be divided into two major thrusts. In the (+)-phorboxazole area, we will: (A) deliver a minimum of one gram of (+)-phorboxazole A employing our now effective second-generation route, in order to make this important agent available for pre-clinical evaluation; (B) exploit the advanced phorboxazole intermediates for a detailed structure-activity study; (C) design and synthesize, guided by the structural activity results, less complex analogs; and (D) prepare chloroacetate, fluorescent, and radiolabeled photoaffinity analogs to define the protein receptor(s), binding site(s), and molecular mechanism(s) of action of this important antitumor agent. In the area of new target molecule/analog synthesis, we will: (E) complete our synthetic strategy for peloruside A; (F) design and synthesize, based on modeling studies, a series of (+)-peloruside A analogs to define the mode of action and binding site(s) of this new tubulin stabilizing antitumor agent; (G) complete the total synthesis of lituarines A, B and C, exploiting a non-aldol paradigm for the construction of polyketide structural units; and (H) initiate a new program directed at the total synthesis of the remarkably potent antitumor agents, (+)-irciniastatin A and B. In each case, the ultimate goal will be to deliver sufficient synthetic material for future biological study. In the area of new reactions/synthetic methods, the specific goals include: (I) develop and explore the scope of the non-aldol tactic to access diverse polyketide fragments of importance to complex molecule synthesis; and (J) demonstrate the utility of the non-aldol tactic for the ready construction of focused libraries based on known natural product scaffolds of biological interest. Beyond these specific synthetic objectives, a general, long-range goal of this program is the identification of the molecular architecture responsible for biological activity. Thus, as we develop an approach to each target structure, we will also prepare model compounds designed to permit the elucidation of structure-activity relationships.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
2R01CA019033-29
Application #
6924472
Study Section
Medicinal Chemistry Study Section (MCHA)
Program Officer
Lees, Robert G
Project Start
1976-06-30
Project End
2009-04-30
Budget Start
2005-05-01
Budget End
2006-04-30
Support Year
29
Fiscal Year
2005
Total Cost
$249,557
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Nguyen, Minh H; Imanishi, Masashi; Kurogi, Taichi et al. (2018) Synthetic Access to the Mandelalide Family of Macrolides: Development of an Anion Relay Chemistry Strategy. J Org Chem 83:4287-4306
Ai, Yanran; Kozytska, Mariya V; Zou, Yike et al. (2018) Total Synthesis of the Marine Phosphomacrolide, (-)-Enigmazole A, Exploiting Multicomponent Type I Anion Relay Chemistry (ARC) in Conjunction with a Late-Stage Petasis-Ferrier Union/Rearrangement. J Org Chem 83:6110-6126
Zou, Yike; Li, Xiangqin; Yang, Yun et al. (2018) Total Synthesis of (-)-Nodulisporic Acids D, C, and B: Evolution of a Unified Synthetic Strategy. J Am Chem Soc 140:9502-9511
Liu, Qi; Deng, Yifan; Smith 3rd, Amos B (2017) Total Synthesis of (-)-Nahuoic Acid Ci (Bii). J Am Chem Soc 139:13668-13671
Liu, Qi; Chen, Yu; Zhang, Xiao et al. (2017) Type II Anion Relay Chemistry: Conformational Constraints To Achieve Effective [1,5]-Vinyl Brook Rearrangements. J Am Chem Soc 139:8710-8717
Nazari, Mohamad; Serrill, Jeffrey D; Wan, Xuemei et al. (2017) New Mandelalides Expand a Macrolide Series of Mitochondrial Inhibitors. J Med Chem 60:7850-7862
Deng, Yifan; Liu, Qi; Smith 3rd, Amos B (2017) Oxidative [1,2]-Brook Rearrangements Exploiting Single-Electron Transfer: Photoredox-Catalyzed Alkylations and Arylations. J Am Chem Soc 139:9487-9490
Montgomery, Thomas D; Smith 3rd, Amos B (2017) ?-Silyl Amides: Effective Bifunctional Lynchpins for Type I Anion Relay Chemistry. Org Lett 19:6216-6219
Nguyen, Minh H; Imanishi, Masashi; Kurogi, Taichi et al. (2016) Total Synthesis of (-)-Mandelalide A Exploiting Anion Relay Chemistry (ARC): Identification of a Type II ARC/CuCN Cross-Coupling Protocol. J Am Chem Soc 138:3675-8
Adams, Gregory L; Smith 3rd, Amos B (2016) The Chemistry of the Akuammiline Alkaloids. Alkaloids Chem Biol 76:171-257

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