A Novel Microbisporicin Producer Identified by Early Dereplication during Lantibiotic Screening
With the increasing need of effective antibiotics against multi-drug resistant pathogens, lantibiotics are an attractive option of a new class of molecules. They are ribosomally synthetized and posttranslationally modified peptides possessing potent antimicrobial activity against aerobic and anaerob...
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doaj-62f561b126ef49ed983a2b3aa8aa80f32020-11-25T00:21:37ZengHindawi LimitedBioMed Research International2314-61332314-61412015-01-01201510.1155/2015/419383419383A Novel Microbisporicin Producer Identified by Early Dereplication during Lantibiotic ScreeningLucia Carrano0Monica Abbondi1Paola Turconi2Gianpaolo Candiani3Flavia Marinelli4Fondazione Istituto Insubrico Ricerca per la Vita (F.I.I.R.V.), Via R. Lepetit 32, 21100 Gerenzano, ItalyFondazione Istituto Insubrico Ricerca per la Vita (F.I.I.R.V.), Via R. Lepetit 32, 21100 Gerenzano, ItalyFondazione Istituto Insubrico Ricerca per la Vita (F.I.I.R.V.), Via R. Lepetit 32, 21100 Gerenzano, ItalyFondazione Istituto Insubrico Ricerca per la Vita (F.I.I.R.V.), Via R. Lepetit 32, 21100 Gerenzano, ItalyDipartimento di Biotecnologie e Scienze della Vita, Università degli Studi dell’Insubria, Via J. H. Dunant 3, 21100 Varese, ItalyWith the increasing need of effective antibiotics against multi-drug resistant pathogens, lantibiotics are an attractive option of a new class of molecules. They are ribosomally synthetized and posttranslationally modified peptides possessing potent antimicrobial activity against aerobic and anaerobic Gram-positive pathogens, including those increasingly resistant to β-lactams and glycopeptides. Some of them (actagardine, mersacidin, planosporicin, and microbisporicin) inhibit cell wall biosynthesis in pathogens and their effect is not antagonized by vancomycin. Hereby, we apply an efficient strategy for lantibiotic screening to 240 members of a newly described genus of filamentous actinomycetes, named Actinoallomurus, that is considered a yet-poorly-exploited promising source for novel bioactive metabolites. By combining antimicrobial differential assay against Staphylococcus aureus and its L-form (also in the presence of a β-lactamase cocktail or Ac-Lys-D-alanyl-D-alanine tripeptide), with LC-UV-MS dereplication coupled with bioautography, a novel producer of the potent microbisporicin complex was rapidly identified. Under the commercial name of NAI-107, it is currently in late preclinical phase for the treatment of multi-drug resistant Gram-positive pathogens. To our knowledge, this is the first report on a lantibiotic produced by an Actinoallomurus sp. and on a microbisporicin producer not belonging to the Microbispora genus.http://dx.doi.org/10.1155/2015/419383 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Lucia Carrano Monica Abbondi Paola Turconi Gianpaolo Candiani Flavia Marinelli |
spellingShingle |
Lucia Carrano Monica Abbondi Paola Turconi Gianpaolo Candiani Flavia Marinelli A Novel Microbisporicin Producer Identified by Early Dereplication during Lantibiotic Screening BioMed Research International |
author_facet |
Lucia Carrano Monica Abbondi Paola Turconi Gianpaolo Candiani Flavia Marinelli |
author_sort |
Lucia Carrano |
title |
A Novel Microbisporicin Producer Identified by Early Dereplication during Lantibiotic Screening |
title_short |
A Novel Microbisporicin Producer Identified by Early Dereplication during Lantibiotic Screening |
title_full |
A Novel Microbisporicin Producer Identified by Early Dereplication during Lantibiotic Screening |
title_fullStr |
A Novel Microbisporicin Producer Identified by Early Dereplication during Lantibiotic Screening |
title_full_unstemmed |
A Novel Microbisporicin Producer Identified by Early Dereplication during Lantibiotic Screening |
title_sort |
novel microbisporicin producer identified by early dereplication during lantibiotic screening |
publisher |
Hindawi Limited |
series |
BioMed Research International |
issn |
2314-6133 2314-6141 |
publishDate |
2015-01-01 |
description |
With the increasing need of effective antibiotics against multi-drug resistant pathogens, lantibiotics are an attractive option of a new class of molecules. They are ribosomally synthetized and posttranslationally modified peptides possessing potent antimicrobial activity against aerobic and anaerobic Gram-positive pathogens, including those increasingly resistant to β-lactams and glycopeptides. Some of them (actagardine, mersacidin, planosporicin, and microbisporicin) inhibit cell wall biosynthesis in pathogens and their effect is not antagonized by vancomycin. Hereby, we apply an efficient strategy for lantibiotic screening to 240 members of a newly described genus of filamentous actinomycetes, named Actinoallomurus, that is considered a yet-poorly-exploited promising source for novel bioactive metabolites. By combining antimicrobial differential assay against Staphylococcus aureus and its L-form (also in the presence of a β-lactamase cocktail or Ac-Lys-D-alanyl-D-alanine tripeptide), with LC-UV-MS dereplication coupled with bioautography, a novel producer of the potent microbisporicin complex was rapidly identified. Under the commercial name of NAI-107, it is currently in late preclinical phase for the treatment of multi-drug resistant Gram-positive pathogens. To our knowledge, this is the first report on a lantibiotic produced by an Actinoallomurus sp. and on a microbisporicin producer not belonging to the Microbispora genus. |
url |
http://dx.doi.org/10.1155/2015/419383 |
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