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Molecular Networking Reveals Two Distinct Chemotypes in Pyrroloiminoquinone-Producing Tsitsikamma favus Sponges

The temperate marine sponge, Tsitsikamma favus, produces pyrroloiminoquinone alkaloids with potential as anticancer drug leads. We profiled the secondary metabolite reservoir of T. favus sponges using HR-ESI-LC-MS/MS-based molecular networking analysis followed by preparative purification efforts to...

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Autores principales: Kalinski, Jarmo-Charles J., Waterworth, Samantha C., Siwe Noundou, Xavier, Jiwaji, Meesbah, Parker-Nance, Shirley, Krause, Rui W. M., McPhail, Kerry L., Dorrington, Rosemary A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6356464/
https://www.ncbi.nlm.nih.gov/pubmed/30654589
http://dx.doi.org/10.3390/md17010060
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author Kalinski, Jarmo-Charles J.
Waterworth, Samantha C.
Siwe Noundou, Xavier
Jiwaji, Meesbah
Parker-Nance, Shirley
Krause, Rui W. M.
McPhail, Kerry L.
Dorrington, Rosemary A.
author_facet Kalinski, Jarmo-Charles J.
Waterworth, Samantha C.
Siwe Noundou, Xavier
Jiwaji, Meesbah
Parker-Nance, Shirley
Krause, Rui W. M.
McPhail, Kerry L.
Dorrington, Rosemary A.
author_sort Kalinski, Jarmo-Charles J.
collection PubMed
description The temperate marine sponge, Tsitsikamma favus, produces pyrroloiminoquinone alkaloids with potential as anticancer drug leads. We profiled the secondary metabolite reservoir of T. favus sponges using HR-ESI-LC-MS/MS-based molecular networking analysis followed by preparative purification efforts to map the diversity of new and known pyrroloiminoquinones and related compounds in extracts of seven specimens. Molecular taxonomic identification confirmed all sponges as T. favus and five specimens (chemotype I) were found to produce mainly discorhabdins and tsitsikammamines. Remarkably, however, two specimens (chemotype II) exhibited distinct morphological and chemical characteristics: the absence of discorhabdins, only trace levels of tsitsikammamines and, instead, an abundance of unbranched and halogenated makaluvamines. Targeted chromatographic isolation provided the new makaluvamine Q, the known makaluvamines A and I, tsitsikammamine B, 14-bromo-7,8-dehydro-3-dihydro-discorhabdin C, and the related pyrrolo-ortho-quinones makaluvamine O and makaluvone. Purified compounds displayed different activity profiles in assays for topoisomerase I inhibition, DNA intercalation and antimetabolic activity against human cell lines. This is the first report of makaluvamines from a Tsitsikamma sponge species, and the first description of distinct chemotypes within a species of the Latrunculiidae family. This study sheds new light on the putative pyrroloiminoquinone biosynthetic pathway of latrunculid sponges.
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spelling pubmed-63564642019-02-05 Molecular Networking Reveals Two Distinct Chemotypes in Pyrroloiminoquinone-Producing Tsitsikamma favus Sponges Kalinski, Jarmo-Charles J. Waterworth, Samantha C. Siwe Noundou, Xavier Jiwaji, Meesbah Parker-Nance, Shirley Krause, Rui W. M. McPhail, Kerry L. Dorrington, Rosemary A. Mar Drugs Article The temperate marine sponge, Tsitsikamma favus, produces pyrroloiminoquinone alkaloids with potential as anticancer drug leads. We profiled the secondary metabolite reservoir of T. favus sponges using HR-ESI-LC-MS/MS-based molecular networking analysis followed by preparative purification efforts to map the diversity of new and known pyrroloiminoquinones and related compounds in extracts of seven specimens. Molecular taxonomic identification confirmed all sponges as T. favus and five specimens (chemotype I) were found to produce mainly discorhabdins and tsitsikammamines. Remarkably, however, two specimens (chemotype II) exhibited distinct morphological and chemical characteristics: the absence of discorhabdins, only trace levels of tsitsikammamines and, instead, an abundance of unbranched and halogenated makaluvamines. Targeted chromatographic isolation provided the new makaluvamine Q, the known makaluvamines A and I, tsitsikammamine B, 14-bromo-7,8-dehydro-3-dihydro-discorhabdin C, and the related pyrrolo-ortho-quinones makaluvamine O and makaluvone. Purified compounds displayed different activity profiles in assays for topoisomerase I inhibition, DNA intercalation and antimetabolic activity against human cell lines. This is the first report of makaluvamines from a Tsitsikamma sponge species, and the first description of distinct chemotypes within a species of the Latrunculiidae family. This study sheds new light on the putative pyrroloiminoquinone biosynthetic pathway of latrunculid sponges. MDPI 2019-01-16 /pmc/articles/PMC6356464/ /pubmed/30654589 http://dx.doi.org/10.3390/md17010060 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Kalinski, Jarmo-Charles J.
Waterworth, Samantha C.
Siwe Noundou, Xavier
Jiwaji, Meesbah
Parker-Nance, Shirley
Krause, Rui W. M.
McPhail, Kerry L.
Dorrington, Rosemary A.
Molecular Networking Reveals Two Distinct Chemotypes in Pyrroloiminoquinone-Producing Tsitsikamma favus Sponges
title Molecular Networking Reveals Two Distinct Chemotypes in Pyrroloiminoquinone-Producing Tsitsikamma favus Sponges
title_full Molecular Networking Reveals Two Distinct Chemotypes in Pyrroloiminoquinone-Producing Tsitsikamma favus Sponges
title_fullStr Molecular Networking Reveals Two Distinct Chemotypes in Pyrroloiminoquinone-Producing Tsitsikamma favus Sponges
title_full_unstemmed Molecular Networking Reveals Two Distinct Chemotypes in Pyrroloiminoquinone-Producing Tsitsikamma favus Sponges
title_short Molecular Networking Reveals Two Distinct Chemotypes in Pyrroloiminoquinone-Producing Tsitsikamma favus Sponges
title_sort molecular networking reveals two distinct chemotypes in pyrroloiminoquinone-producing tsitsikamma favus sponges
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6356464/
https://www.ncbi.nlm.nih.gov/pubmed/30654589
http://dx.doi.org/10.3390/md17010060
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