Abstract

Natural product research during the last few decades has yielded thousands of novel, bioactive organic compounds from the marine environment. However, little has been done to explore the application of marine natural products for the treatment of the AIDS opportunistic infections Mycobacterium sp. The primary goal of this project is the gram scale isolation of those marine structural classes identified as having significant activity against Mycobacterium in vitro. The natural product scaffolds will be utilized for biological evaluation, structural modifications and lead optimization, The marine natural products of interest include: manzamine alkaloids; uranidine alkaloids; C19 hydroxy steroids; tetrabromo spirocyclohexadienylisoxazolines; scalarin sesterterpenoids and shikimate-sesquiterpenes. The isolation and structure determination of both the major and minor natural product constituents of these marine structural classes will be completed. Pure natural, semisynthetic and biotransformation products from these six unique structural classes will be evaluated for biological activity at the Tuberculosis Antimicrobial Acquisition & Coordinating Facilities (TAACF). Lead optimization studies of the active scaffolds isolated in 50mg or greater quantities (1 gram target isolation) will be completed using combinatorial/parallel synthesis and microbial transformations (including combinatorial). The marine natural products will be purified using preparative and semi-preparative high pressure liquid chromatography (HPLC), independently and interfaced with NMR and FTMS. The chemical structures of biologically active products will be determined with the use of 2D NMR and FTMS. Structure activity relationships (SAR) will be completed using the biological results generated from natural, semisynthetic and bioconversion products. In addition the microbial metabolism studies will provide valuable information regarding the metabolic fate of these lead marine derived anti-TB structural classes. Optimized marine natural product derived leads will be scaled-up for in vivo anti-TB assays in mice. Tuberculosis is an extremely serious disease infecting an estimated one-third of the world's population. The rapid spread of drug-resistant strains of this bacillus in the last several years has created an urgent need for novel therapeutic agents with new modes of action to counter this impending threat. The six marine-derived structural classes described in this proposal will undergo thorough preclinical evaluation to determine their potential as drug leads for the treatment of TB.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI036596-08
Application #
6631863
Study Section
AIDS and Related Research 8 (AARR)
Program Officer
Lambros, Chris
Project Start
1995-04-01
Project End
2004-05-31
Budget Start
2003-06-01
Budget End
2004-05-31
Support Year
8
Fiscal Year
2003
Total Cost
$322,875
Indirect Cost

  Institution

Name
University of Mississippi
Department
Pharmacology
Type
Schools of Pharmacy
DUNS #
067713560
City
University
State
MS
Country
United States
Zip Code
38677

  Publications

Gogineni, Vedanjali; Hamann, Mark T (2018) Marine natural product peptides with therapeutic potential: Chemistry, biosynthesis, and pharmacology. Biochim Biophys Acta Gen Subj 1862:81-196
Wang, Bin; Waters, Amanda L; Valeriote, Frederick A et al. (2015) An efficient and cost-effective approach to kahalalide F N-terminal modifications using a nuisance algal bloom of Bryopsis pennata. Biochim Biophys Acta 1850:1849-54
Kasanah, Noer; Farr, Lorelei Lucas; Gholipour, Abbas et al. (2014) Metabolism and resistance of Fusarium spp. to the manzamine alkaloids via a putative retro pictet-spengler reaction and utility of the rational design of antimalarial and antifungal agents. Mar Biotechnol (NY) 16:412-22
Li, Huayue; Su, Mingzhi; Hamann, Mark T et al. (2014) Solution structure of a sponge-derived cystine knot peptide and its notable stability. J Nat Prod 77:304-10
Waters, Amanda L; Peraud, Olivier; Kasanah, Noer et al. (2014) An analysis of the sponge Acanthostrongylophora igens' microbiome yields an actinomycete that produces the natural product manzamine A. Front Mar Sci 1:
Li, Huayue; Bowling, John J; Fronczek, Frank R et al. (2013) Asteropsin A: an unusual cystine-crosslinked peptide from porifera enhances neuronal Ca2+ influx. Biochim Biophys Acta 1830:2591-9
Olugbuyiro, J A O; Moody, J O; Hamann, M T (2013) Phytosterols from Spondias mombin Linn with Antimycobacterial Activities. Afr J Biomed Res 16:19-24
Hwang, In Hyun; Oh, Joonseok; Kochanowska-Karamyan, Anna et al. (2013) A novel natural phenyl alkene with cytotoxic activity. Tetrahedron Lett 54:3872-3876
Zou, Yike; Hamann, Mark T (2013) Atkamine: a new pyrroloiminoquinone scaffold from the cold water Aleutian Islands Latrunculia sponge. Org Lett 15:1516-9
Wahba, Amir E; Fromentin, Yann; Zou, Yike et al. (2012) Acantholactone, a new manzamine related alkaloid with an unprecedented ?-lactone and ?-lactam ring system. Tetrahedron Lett 53:6329-6331

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