Bioactive secondary metabolites from marine and under explored habitats

This thesis presents results obtained from the investigation of secondary metabolites through screening of marine organisms, marine-derived microbes, and microbes form under-explored habitats. The first part includes the isolation of eight cytotoxic diterpene derivatives of which four were new from...

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Main Author: Rateb, Mostafa Ezzat M.
Published: University of Aberdeen 2011
Subjects:
Online Access:http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.542654
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spelling ndltd-bl.uk-oai-ethos.bl.uk-5426542015-03-20T04:06:58ZBioactive secondary metabolites from marine and under explored habitatsRateb, Mostafa Ezzat M.2011This thesis presents results obtained from the investigation of secondary metabolites through screening of marine organisms, marine-derived microbes, and microbes form under-explored habitats. The first part includes the isolation of eight cytotoxic diterpene derivatives of which four were new from the organic extract of the sponge <i>Spongionella </i>sp. obtained from the U.S. National Cancer Institute’s Open Repository Program, the isolation of three new antibacterial dibenzofuran derivatives and a known butyrolactone from ascomycete Super1F1-09 isolated from the Indo-Pacific sponge <i>Acanthella cavernosa. </i>An attempt to synthesize these compounds was conducted. This part also includes the isolation of five known pyrroloiminoquinone alkaloids, from the Fijian sponge <i>Zyzzya</i> sp., which showed potent antiprotozoal activity. The second part comprises the use of OSMAC approach for the isolation of four new ansamycin-type polyketides, three new macrolactones and one known siderophore from <i>Streptomyces </i>strain C34 isolated from Atacama Desert, Chile. These compounds showed good antibacterial activity with one of the ansamycins showed pronounced antibacterial activity against a panel of clinical isolates of methicillin-sensitive as well as methicillin-resistant <i>S. aureus</i> (MRSA). This part also contains the use of microbial co-culture for the induction of secondary metabolites. It comprises the isolation of ten antiprotozoal fungal metabolites, of which one was new, from <i>Aspergillus fumigatus </i>when co-cultured with the novel strain <i>Streptomyces </i>C2 isolated from Atacama Desert. In conclusion, natural products from diverse sources proved to be the major resource of drug discovery. This thesis describes the isolation and structural characterisation of 35 compounds, 15 of which were new. Extremophiles proved to be a good source for new secondary metabolites.615.321Metabolites : Marine organismsUniversity of Aberdeenhttp://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.542654http://digitool.abdn.ac.uk:80/webclient/DeliveryManager?pid=167782Electronic Thesis or Dissertation
collection NDLTD
sources NDLTD
topic 615.321
Metabolites : Marine organisms
spellingShingle 615.321
Metabolites : Marine organisms
Rateb, Mostafa Ezzat M.
Bioactive secondary metabolites from marine and under explored habitats
description This thesis presents results obtained from the investigation of secondary metabolites through screening of marine organisms, marine-derived microbes, and microbes form under-explored habitats. The first part includes the isolation of eight cytotoxic diterpene derivatives of which four were new from the organic extract of the sponge <i>Spongionella </i>sp. obtained from the U.S. National Cancer Institute’s Open Repository Program, the isolation of three new antibacterial dibenzofuran derivatives and a known butyrolactone from ascomycete Super1F1-09 isolated from the Indo-Pacific sponge <i>Acanthella cavernosa. </i>An attempt to synthesize these compounds was conducted. This part also includes the isolation of five known pyrroloiminoquinone alkaloids, from the Fijian sponge <i>Zyzzya</i> sp., which showed potent antiprotozoal activity. The second part comprises the use of OSMAC approach for the isolation of four new ansamycin-type polyketides, three new macrolactones and one known siderophore from <i>Streptomyces </i>strain C34 isolated from Atacama Desert, Chile. These compounds showed good antibacterial activity with one of the ansamycins showed pronounced antibacterial activity against a panel of clinical isolates of methicillin-sensitive as well as methicillin-resistant <i>S. aureus</i> (MRSA). This part also contains the use of microbial co-culture for the induction of secondary metabolites. It comprises the isolation of ten antiprotozoal fungal metabolites, of which one was new, from <i>Aspergillus fumigatus </i>when co-cultured with the novel strain <i>Streptomyces </i>C2 isolated from Atacama Desert. In conclusion, natural products from diverse sources proved to be the major resource of drug discovery. This thesis describes the isolation and structural characterisation of 35 compounds, 15 of which were new. Extremophiles proved to be a good source for new secondary metabolites.
author Rateb, Mostafa Ezzat M.
author_facet Rateb, Mostafa Ezzat M.
author_sort Rateb, Mostafa Ezzat M.
title Bioactive secondary metabolites from marine and under explored habitats
title_short Bioactive secondary metabolites from marine and under explored habitats
title_full Bioactive secondary metabolites from marine and under explored habitats
title_fullStr Bioactive secondary metabolites from marine and under explored habitats
title_full_unstemmed Bioactive secondary metabolites from marine and under explored habitats
title_sort bioactive secondary metabolites from marine and under explored habitats
publisher University of Aberdeen
publishDate 2011
url http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.542654
work_keys_str_mv AT ratebmostafaezzatm bioactivesecondarymetabolitesfrommarineandunderexploredhabitats
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