Lincomycin at Subinhibitory Concentrations Potentiates Secondary Metabolite Production by Streptomyces spp

Imai, Yu; Sato, Seizo; Tanaka, Yukinori; Ochi, Kozo; Hosaka, Takeshi

doi:10.1128/aem.04214-14

Cited by 59 publications

(48 citation statements)

References 55 publications

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“…This was the case with tetracycline and lincomycin (Shima et al 1996;Imai et al 2015). It will be interesting to see what the mechanism of induced secondary metabolite production is in these non-resistant strains, a case that is akin to examples of goadsporin or promomycin in coculture experiments.…”

Section: Mechanismmentioning

confidence: 99%

Antibiotic dialogues: induction of silent biosynthetic gene clusters by exogenous small molecules

Okada¹,

Seyedsayamdost²

2016

FEMS Microbiology Reviews

170

150

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One sentence summary: Microbial secondary metabolites represent a significant source of potential drug leads; however, the majority of the corresponding biosynthetic genes are not expressed under normal laboratory conditions. In this review, we assess the capacity of exogenous small molecules, especially antibiotics, to activate these silent gene clusters. Editor: Aimee Shen ABSTRACTNatural products have traditionally served as a dominant source of therapeutic agents. They are produced by dedicated biosynthetic gene clusters that assemble complex, bioactive molecules from simple precursors. Recent genome sequencing efforts coupled with advances in bioinformatics indicate that the majority of biosynthetic gene clusters are not expressed under normal laboratory conditions. Termed 'silent' or 'cryptic', these gene clusters represent a treasure trove for discovery of novel small molecules, their regulatory circuits and their biosynthetic pathways. In this review, we assess the capacity of exogenous small molecules in activating silent secondary metabolite gene clusters. Several approaches that have been developed are presented, including coculture techniques, ribosome engineering, chromatin remodeling and high-throughput elicitor screens. The rationale, applications and mechanisms attendant to each are discussed. Some general conclusions can be drawn from our analysis: exogenous small molecules comprise a productive avenue for the discovery of cryptic metabolites. Specifically, growth-inhibitory molecules, in some cases clinically used antibiotics, serve as effective inducers of silent biosynthetic gene clusters, suggesting that old antibiotics may be used to find new ones. The involvement of natural antibiotics in modulating secondary metabolism at subinhibitory concentrations suggests that they represent part of the microbial vocabulary through which inter-and intraspecies interactions are mediated.

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Section: Mechanismmentioning

confidence: 99%

Antibiotic dialogues: induction of silent biosynthetic gene clusters by exogenous small molecules

Okada¹,

Seyedsayamdost²

2016

FEMS Microbiology Reviews

170

150

View full text Add to dashboard Cite

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“…Antibiotics at sublethal concentrations can generate diverse metabolic responses in bacteria (Imai et al, 2015). Identification of elicitors that induce the expression of silent gene clusters under standard conditions is however a challenge.…”

Section: Elicitation With Microbial Cell Componentsmentioning

confidence: 99%

Elicitation of secondary metabolism in actinomycetes

Abdelmohsen

Grkovic

Balasubramanian

et al. 2015

Biotechnology Advances

206

158

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Genomic sequence data have revealed the presence of a large fraction of putatively silent biosynthetic gene clusters in the genomes of actinomycetes that encode for secondary metabolites, which are not detected under standard fermentation conditions. This review focuses on the effects of biological (co-cultivation), chemical, as well as molecular elicitation on secondary metabolism in actinomycetes. Our review covers the literature until June 2014 and exemplifies the diversity of natural products that have been recovered by such approaches from the phylum Actinobacteria.

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“…After induction at 37°C for 4 h, the cells were collected by centrifugation and resuspended in fresh LB broth to an OD 600 of ϳ1.0. A 20-l aliquot of each was inoculated onto LB plates containing ampicillin (100 g/ml), IPTG (50 g/ml), and lincomycin (200 g/ml), followed by incubation at 37°C for 24 h. centrations of lincomycin (1/16 to 1/4 of its MIC) in the culture medium markedly enhanced ACT production by S. coelicolor (38), although the mechanism underlying this ACT overproduction appears different from that of the two-component system. Thus, the acquisition of lincomycin resistance by certain spontaneous mutations and the addition of lincomycin into the medium both could be effective at activating or enhancing antibiotic production in actinomycetes.…”

Section: Discussionmentioning

confidence: 99%

Identification of a Novel Lincomycin Resistance Mutation Associated with Activation of Antibiotic Production in Streptomyces coelicolor A3(2)

Wang

Izawa

Yang

et al. 2017

Antimicrob Agents Chemother

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Comparative genome sequencing analysis of a lincomycin-resistant strain of Streptomyces coelicolor A3(2) and the wild-type strain identified a novel mutation conferring a high level of lincomycin resistance. Surprisingly, the new mutation was an in-frame DNA deletion in the genes SCO4597 and SCO4598, resulting in formation of the hybrid gene linR. SCO4597 and SCO4598 encode two histidine kinases, which together with SCO4596, encoding a response regulator, constitute a unique twocomponent system. Sequence analysis indicated that these three genes and their arrangement patterns are ubiquitous among all Streptomyces genomes sequenced to date, suggesting these genes play important regulatory roles. Gene replacement showed that this mutation was responsible for the high level of lincomycin resistance, the overproduction of the antibiotic actinorhodin, and the enhanced morphological differentiation of this strain. Moreover, heterologous expression of the hybrid gene linR in Escherichia coli conferred resistance to lincomycin in this organism. Introduction of the hybrid gene linR in various Streptomyces strains by gene engineering technology may widely activate and/or enhance antibiotic production.

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Lincomycin at Subinhibitory Concentrations Potentiates Secondary Metabolite Production by Streptomyces spp

Cited by 59 publications

References 55 publications

Antibiotic dialogues: induction of silent biosynthetic gene clusters by exogenous small molecules

Antibiotic dialogues: induction of silent biosynthetic gene clusters by exogenous small molecules

Elicitation of secondary metabolism in actinomycetes

Identification of a Novel Lincomycin Resistance Mutation Associated with Activation of Antibiotic Production in Streptomyces coelicolor A3(2)

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