Fermentative production of self-toxic fungal secondary metabolites

Singh, Manpreet; Leighton, Margaret; Barbieri, Laurel R.; Roll, Deborah M.; Urbance, Susan E.; Hoshan, Linda; McDonald, Leonard A.

doi:10.1007/s10295-009-0678-9

Cited by 36 publications

(26 citation statements)

References 21 publications

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“…According to previous reports that the metal ions, secondary metabolism activators, and extractive resins had effects on the production of natural products [8,9,12,13,19]. In this work, HPLC-DAD quantification [13] and the two known activators salicylic acid (SA) and methyl jasmonate (MeJA) showed slight or adverse effects on CPT production (Fig.…”

mentioning

confidence: 56%

Isolation and characterization of Paenibacillus polymyxa LY214, a camptothecin-producing endophytic bacterium from Camptotheca acuminata

Xiang

Chen

Yang

et al. 2015

Journal of Industrial Microbiology and Biotechnology

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Camptothecin (CPT) is mainly produced and extracted from Camptotheca acuminata and Nothapodytes foetida for pharmaceutical use, i.e., the starting material for chemical conversion to the clinical CPT-type drugs. As the third largest plant anticancer drug, the heavy demand on CPT from global market leads to many research efforts to identify new sources for CPT production. Herein we report the isolation and characterization of a CPT-producing endophytic bacterium Paenibacillus polymyxa LY214 from Camptotheca acuminata. A 10.7 μg l−1 of CPT was presented in the fermentation broth of P. polymyxa LY214. Its CPT production decreased sharply when the strain of the 2nd generation of P. polymyxa LY214 was cultured and fermented. However, the CPT production remained relatively constant from 2.8 μg l−1 of the 2nd generation to 0.8 μg l−1 of the 8th generation of P. polymyxa LY214 under optimized fermentation conditions. A 15- to 30-fold increase of CPT yield was observed when the optimized fermentation conditions, together with the addition of putative biosynthetic precursors of CPT and adsorbent resin XAD16, were applied to ferment the strains of the 7th and 8th generation of P. polymyxa LY214. Bioinformatics analysis of the relative species of P. polymyxa LY214 indicates its potential to produce CPT, which will be helpful to decipher the mysteries of CPT biosynthesis.

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mentioning

confidence: 56%

Isolation and characterization of Paenibacillus polymyxa LY214, a camptothecin-producing endophytic bacterium from Camptotheca acuminata

Xiang

Chen

Yang

et al. 2015

Journal of Industrial Microbiology and Biotechnology

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“…Among them, MeJA is an optimum elicitor in view of that CPT yield increased 3.4-fold. Additionally, end-product feedback inhibition is another common problem during fermentation processes when the concentration of the end product reaches a certain level (Singh et al 2010;Parawira and Tekere 2011). Inclusion of an adsorbent resin in the production medium in combination with extractive fermentation is an effective approach to reduce end-product feedback inhibition and to increase the product titer.…”

Section: Discussionmentioning

confidence: 99%

“…Inclusion of an adsorbent resin in the production medium in combination with extractive fermentation is an effective approach to reduce end-product feedback inhibition and to increase the product titer. For instance, successes have been made by using HP20 in bacterium fermentation to improve the concentration of anticancer compound thailandepsin A (Liu et al 2012) or to reduce the self-toxicity of the fungal metabolite (Singh et al 2010). We speculated that this approach might be useful to improve CPT yield in LY357.…”

Section: Discussionmentioning

confidence: 99%

Camptothecin-producing endophytic fungus Trichoderma atroviride LY357: isolation, identification, and fermentation conditions optimization for camptothecin production

Xiang

Xing

Chen

et al. 2013

Appl Microbiol Biotechnol

148

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Camptothecin (CPT), the third largest anticancer drug, is produced mainly by Camptotheca acuminata and Nothapodytes foetida. CPT itself is the starting material for clinical CPT-type drugs, but the plant-derived CPT cannot support the heavy demand from the global market. Research efforts have been made to identify novel sources for CPT. In this study, three CPT-producing endophytic fungi, Aspergillus sp. LY341, Aspergillus sp. LY355, and Trichoderma atroviride LY357, were isolated and identified from C. acuminata. Most CPT produced by these fungi was found in the fermentation broth, and their corresponding CPT yields were 7. 93, 42.92, and 197.82 μg l −1 , respectively. The CPT-producing capability of LY341 and LY355 was completely lost after repeat subculturing. A substantial decrease of CPT production was also observed in the second generation of LY357. However, a stable and sustainable production of CPT was found from the second generation through the eighth generation of LY357. The fermentation medium, time, pH, temperature, and agitation rate were optimized for CPT production. Methyl jasmonate and XAD16 were proven to be an optimum elicitor and adsorbent resin, respectively, in view of that CPT yield was increased 3.4-and 11-fold through their use. A 50-to 75-fold increase of CPT yield was obtained when the optimized fermentation conditions, elicitor, and adsorbent resin were combined and applied to the culture of the seventh and eighth generations of LY357, and the highest CPT yield was 142.15 μg l −1 . The CPTproducing T. atroviride LY357 paves a potential to uncover the mysteries of CPT biosynthesis.

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“…Because the concentration of a precursor during the fermentation varies in dependence on its dosage intervals, we added into the fermentor adsorbent resin, which keeps the precursor concentration relatively constant by reversibly adsorbing and releasing it. 18,19 The optimum resin concentration in our experiments was 10 g l À1 .…”

Section: Precursor-directed Biosynthesismentioning

confidence: 92%

Pilot-plant cultivation of Streptomyces griseus producing homologues of nonactin by precursor-directed biosynthesis and their identification by LC/MS-ESI

et al. 2010

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Precursor-directed biogenetic approach was used to produce a range of nonactin homologues in a 50 l fermentor cultivation of strain Streptomyces griseus 34/249 obtained by UV mutagenesis. The production medium contained sodium propionate, isobutyrate and isovalerate as individual precursors, and 10 g l À1 Diaion HP20 styrene-divinylbenzene resin that maintains suitable precursor concentration by reversibly adsorbing and releasing it. The produced nonactin homologues were separated on two C18 reversed-phase liquid chromatography columns in series and analyzed by MS with ESI source in the positive ion mode. Formation of doubly charged ions was suppressed by an excess of Na + ions throughout the process. The production of the homologues increased up to day 5 and then it leveled off. Cultivations with individual precursors yielded a total of 18 nonactin homologues whose spectrum depended on the precursor used. The total production of the homologues was lowered but their spectrum was shifted to higher-molecular-weight compounds.

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Fermentative production of self-toxic fungal secondary metabolites

Cited by 36 publications

References 21 publications

Isolation and characterization of Paenibacillus polymyxa LY214, a camptothecin-producing endophytic bacterium from Camptotheca acuminata

Isolation and characterization of Paenibacillus polymyxa LY214, a camptothecin-producing endophytic bacterium from Camptotheca acuminata

Camptothecin-producing endophytic fungus Trichoderma atroviride LY357: isolation, identification, and fermentation conditions optimization for camptothecin production

Pilot-plant cultivation of Streptomyces griseus producing homologues of nonactin by precursor-directed biosynthesis and their identification by LC/MS-ESI

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