Abstract

The research is directed toward the design and development of general strategies for the syntheses of oxygenated natural and unnatural products possessing biological activity. The investigation of synthetic applications of dipolar cycloadditions involving nitrile oxides will be continued. Another area of current interest will be in the extension of a general synthetic strategy that features the use of substituted furans as latent 1,4-dicarbonyl compounds and as highly useful intermediates for the stereoselective construction of functionalized hydropyrans, hydroxylated piperidines, and other important oxygenated cyclic and acyclic synthons. The methodology, which is developed during the course of these studies, will be applied to the total syntheses of: (a) the erythronolides A and B, the aglycones of the medicinally important macrolide antibiotics erythromycins A and B; (b) tylonolide, the aglycone of the macrolide antibiotic tylosin; (c) phyllanthocin, the aglycone of the antileukemic and antimelanoma glycoside phyllanthoside; (d) the pseudomonic acids A, B, and C, important antibiotics and antimicrobial agents, which are also competitive inhibitors of isoleucyl-tRNA synthetase; (e) the higher monosaccharides KDO, an eight carbon sugar that links the lipid section to the interior carbohydrate section of lipopolysaccharides of Gram-negative bacteria, and lincosamine, the saccharide subunit of the clinically important antibiotic lincomycin; (f) the polyhydroxylated alkaloids including nojirimycin, 1-deoxynor-jirimycin, 2(S)-carboxy-3(R),4(R),5(S)-trihydroxypiperidine, nojirimycin B and 1-deoxymannojirimycin, which have been shown to inhibit the glycosidases and mannosidases involved in the processing pathways that result in oligosaccharide maturation; and (g) breynogenin, an aglycone of the breynins A and B, sulfur containing glycosides that exhibit significant hypocholesterolemic activity. Reasonable quantities of selected synthetic intermediates and analogues of the above natural products for biological screening. Agreements to test various compounds for biological activity have been established with McNeil Laboratories, the Upjohn Company, Shell Development Laboratories and Chevron Chemical Company, all of which have already screened compounds from other NIH supported projects. Those substances which might exhibit anticancer activity will be submitted to the National Cancer Institute for evaluation as potential anticancer agents.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
2R01GM031077-04
Application #
3278972
Study Section
Bio-Organic and Natural Products Chemistry Study Section (BNP)
Project Start
1983-06-01
Project End
1989-07-31
Budget Start
1986-08-01
Budget End
1987-07-31
Support Year
4
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
University of Texas Austin
Department
Type
Schools of Arts and Sciences
DUNS #
City
Austin
State
TX
Country
United States
Zip Code
78713

  Publications

Klosowski, Daniel W; Martin, Stephen F (2018) Synthesis of (+)-Disparlure via Enantioselective Iodolactonization. Org Lett 20:1269-1271
Klosowski, Daniel W; Hethcox, J Caleb; Paull, Daniel H et al. (2018) Enantioselective Halolactonization Reactions using BINOL-Derived Bifunctional Catalysts: Methodology, Diversification, and Applications. J Org Chem 83:5954-5968
Martin, Stephen F (2017) Natural Products and Their Mimics as Targets of Opportunity for Discovery. J Org Chem 82:10757-10794
Hethcox, J Caleb; Shanahan, Charles S; Martin, Stephen F (2015) Diastereoselective addition of monoorganocuprates to a chiral fumarate: reaction development and synthesis of (-)-dihydroprotolichesterinic acid. Tetrahedron 71:6361-6368
Yang, Jingyue; Knueppel, Daniel; Cheng, Bo et al. (2015) Approaches to polycyclic 1,4-dioxygenated xanthones. Application to total synthesis of the aglycone of IB-00208. Org Lett 17:114-7
Knueppel, Daniel; Yang, Jingyue; Cheng, Bo et al. (2015) Total Synthesis of the Aglycone of IB-00208. Tetrahedron 71:5741-5757
Shanahan, Charles S; Fang, Chao; Paull, Daniel H et al. (2013) Asymmetric Formal Total Synthesis of the Stemofoline Alkaloids: The Evolution, Development and Application of a Catalytic Dipolar Cycloaddition Cascade. Tetrahedron 69:7592-7607
Fang, Chao; Paull, Daniel H; Hethcox, J Caleb et al. (2013) Enantioselective iodolactonization of disubstituted olefinic acids using a bifunctional catalyst. Org Lett 15:972
Fang, Chao; Shanahan, Charles S; Paull, Daniel H et al. (2012) Enantioselective formal total syntheses of didehydrostemofoline and isodidehydrostemofoline through a catalytic dipolar cycloaddition cascade. Angew Chem Int Ed Engl 51:10596-9
Fang, Chao; Paull, Daniel H; Hethcox, J Caleb et al. (2012) Enantioselective iodolactonization of disubstituted olefinic acids using a bifunctional catalyst. Org Lett 14:6290-3

Showing the most recent 10 out of 53 publications