Abstract

Azaspiracid is a potently toxic natural product that represents a human health hazard due to its seasonal contamination of mussels (Mytilus edulis) that have been cultivated for human consumption. This unique toxin was isolated recently from Irish mussels (2 mg/20 kg mussel tissue) and is responsible for the acute poisoning of several humans. The structure of azaspiracid has been only partially assigned on the basis of spectroscopic studies, but the actual structure may be one of four possible isomers. Azaspiracid is an 842 MW. omega-amino acid with a 40 carbon backbone that is punctuated by an unprecedented array of two fused polycyclic domains connected via a 2,6-disubstituted pyranyl hemiketal and terminating in a spiroaminal. The lethal dose in mice was determined to be 0.2 mg/kg (i.p. injection). Although the mechanism of action remains to be explored, azaspiracid does not inhibit the protein serine/threonine phosphatase 2A that is affected by other diarrhetic shellfish toxins. The complex yet undefined structure of azaspiracid, coupled with its potent vertebrate toxicity, presents unique opportunities for synthetic, structural, and biological study. The primary goals of this proposal are to develop and apply novel synthetic strategies for the rapid and convergent assembly of azaspiracid's component polycyclic domains, and to utilize these synthetic products to assign the complete structure of the natural product and provide an alternative source via total synthesis for further biological evaluation and environmental monitoring. Azaspiracid has been retrosynthetically divided into two major domains representing carbons 1-20 and 21-40 of the natural product. The C1-C20 portion of azaspiracid contains 8 stereogenic centers and is comprised of a tetrahydrofuran-fused 6-5-6 trioxaspirotetracyclic ring system (rings A-B-C-D) that is linked via a single acyclic carbinol carbon (C20) to a hemiketal, pyranyl E ring. The spiro-fused A-B-C ring system is representative of similar structural motifs in several other biologically active natural products. It will be assembled in a novel convergent approach that involves the nucleophilic coupling of an A-B ring precursor with a C-D ring lactone, followed by an acid triggered transketalization to close the B ring and complete the trioxaspiroketal system. The C21-C40 domain of azaspiracid consists of the isolated hemiketal E ring and the unique spiroaminal-fused 2,9-dioxabicyclo(3.3.1)nonane ring system (rings F-G-H-I) and contains 12 stereogenic centers. The F-I system presents an opportunity to develop a novel, biomimetic polycyclization cascade sequence that will provide unique synthetic access to this polycyclic array that will be instrumental for assigning the stereochemistry and developing a total synthesis of the natural product.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
5R01ES010615-03
Application #
6525229
Study Section
Medicinal Chemistry Study Section (MCHA)
Program Officer
Lawler, Cindy P
Project Start
2000-08-15
Project End
2003-07-31
Budget Start
2002-08-01
Budget End
2003-07-31
Support Year
3
Fiscal Year
2002
Total Cost
$287,264
Indirect Cost

  Institution

Name
University of Minnesota Twin Cities
Department
Chemistry
Type
Other Domestic Higher Education
DUNS #
168559177
City
Minneapolis
State
MN
Country
United States
Zip Code
55455

  Publications

Zhang, Zhigao; Chen, Yong; Adu-Ampratwum, Daniel et al. (2016) Synthesis of the C22-C40 Domain of the Azaspiracids. Org Lett 18:1824-7
Samdal, Ingunn A; Løvberg, Kjersti E; Briggs, Lyn R et al. (2015) Development of an ELISA for the Detection of Azaspiracids. J Agric Food Chem 63:7855-61
Zhang, Zhigao; Ding, Yue; Xu, Jianyan et al. (2013) Synthesis of the C1-C21 domain of azaspiracids-1 and -3. Org Lett 15:2338-41
Fang, Chao; Pang, Yucheng; Forsyth, Craig J (2010) Formal total synthesis of okadaic acid via regiocontrolled gold(I)-catalyzed spiroketalizations. Org Lett 12:4528-31
Trygstad, Timothy M; Pang, Yucheng; Forsyth, Craig J (2009) Versatile synthesis of the C3-C14 domain of 7-deoxyokadaic acid. J Org Chem 74:910-3
Li, Yongfeng; Zhou, Feng; Forsyth, Craig J (2007) Gold(I)-catalyzed bis-spiroketalization: synthesis of the trioxadispiroketal-containing A-D rings of azaspiracid. Angew Chem Int Ed Engl 46:279-82
Forsyth, Craig J; Xu, Jianyan; Nguyen, Son T et al. (2006) Antibodies with broad specificity to azaspiracids by use of synthetic haptens. J Am Chem Soc 128:15114-6
Wang, Ce; Forsyth, Craig J (2006) Synthesis of the spirastrellolide A trioxadispiroketal. Org Lett 8:2997-3000
Geisler, Lisa K; Nguyen, Son; Forsyth, Craig J (2004) Synthesis of the azaspiracid-1 trioxadispiroketal. Org Lett 6:4159-62
Dounay, A B; Forsyth, C J (2001) Synthetic studies toward the C5-C20 domain of the azaspiracids. Org Lett 3:975-8

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