Production of novel fusarielins by ectopic activation of the polyketide synthase 9 cluster in Fusarium graminearum.

Jens Laurids Sørensen; Frederik Teilfeldt Hansen; Teis Søndergaard; Dan Staerk; Tet V. Lee; Reinhard Wimmer; Louise G. Klitgaard; Stig Purup; Henriette Giese; Rasmus John Nordmand Frandsen

doi:10.1111/j.1462-2920.2011.02696.x

Production of novel fusarielins by ectopic activation of the polyketide synthase 9 cluster in Fusarium graminearum.

Jens Laurids Sørensen, Frederik Teilfeldt Hansen, Teis Søndergaard, Dan Staerk, Tet V. Lee, Reinhard Wimmer, Louise G. Klitgaard, Stig Purup, Henriette Giese, Rasmus John Nordmand Frandsen

Institut for Kemi og Biovidenskab

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

62 Citationer (Scopus)

Abstract

Like many other filamentous fungi, Fusarium graminearum has the genetic potential to produce a vast array of unknown secondary metabolites. A promising approach to determine the nature of these is to activate silent secondary metabolite gene clusters through constitutive expression of cluster specific transcription factors. We have developed a system in which an expression cassette containing the transcription factor from the targeted PKS cluster disrupts the production of the red mycelium pigment aurofusarin. This aids with identification of mutants as they appear as white colonies and metabolite analyses where aurofusarin and its intermediates are normally among the most abundant compounds. The system was used for constitutive expression of the local transcription factor from the PKS9 cluster (renamed FSL) leading to production of three novel fusarielins, F, G and H. This group of compounds has not previously been reported from F. graminearum or linked to a biosynthetic gene in any fungal species. The toxicity of the three novel fusarielins was examined against colorectal cancer cell lines where fusarielin H was more potent than fusarielin F and G.

Originalsprog	Engelsk
Tidsskrift	Environmental Microbiology
Vol/bind	14
Udgave nummer	5
Sider (fra-til)	1159-1170
ISSN	1462-2912
DOI	https://doi.org/10.1111/j.1462-2920.2011.02696.x
Status	Udgivet - maj 2012

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Citationsformater

Sørensen, J. L., Hansen, F. T., Søndergaard, T., Staerk, D., V. Lee, T., Wimmer, R., G. Klitgaard, L., Purup, S., Giese, H., & John Nordmand Frandsen, R. (2012). Production of novel fusarielins by ectopic activation of the polyketide synthase 9 cluster in Fusarium graminearum. Environmental Microbiology, 14(5), 1159-1170. https://doi.org/10.1111/j.1462-2920.2011.02696.x

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title = "Production of novel fusarielins by ectopic activation of the polyketide synthase 9 cluster in Fusarium graminearum.",

abstract = "Like many other filamentous fungi, Fusarium graminearum has the genetic potential to produce a vast array of unknown secondary metabolites. A promising approach to determine the nature of these is to activate silent secondary metabolite gene clusters through constitutive expression of cluster specific transcription factors. We have developed a system in which an expression cassette containing the transcription factor from the targeted PKS cluster disrupts the production of the red mycelium pigment aurofusarin. This aids with identification of mutants as they appear as white colonies and metabolite analyses where aurofusarin and its intermediates are normally among the most abundant compounds. The system was used for constitutive expression of the local transcription factor from the PKS9 cluster (renamed FSL) leading to production of three novel fusarielins, F, G and H. This group of compounds has not previously been reported from F. graminearum or linked to a biosynthetic gene in any fungal species. The toxicity of the three novel fusarielins was examined against colorectal cancer cell lines where fusarielin H was more potent than fusarielin F and G.",

author = "S{\o}rensen, {Jens Laurids} and Hansen, {Frederik Teilfeldt} and Teis S{\o}ndergaard and Dan Staerk and {V. Lee}, Tet and Reinhard Wimmer and {G. Klitgaard}, Louise and Stig Purup and Henriette Giese and {John Nordmand Frandsen}, Rasmus",

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doi = "10.1111/j.1462-2920.2011.02696.x",

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Sørensen, JL, Hansen, FT, Søndergaard, T, Staerk, D, V. Lee, T, Wimmer, R, G. Klitgaard, L, Purup, S, Giese, H & John Nordmand Frandsen, R 2012, 'Production of novel fusarielins by ectopic activation of the polyketide synthase 9 cluster in Fusarium graminearum.', Environmental Microbiology, bind 14, nr. 5, s. 1159-1170. https://doi.org/10.1111/j.1462-2920.2011.02696.x

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T1 - Production of novel fusarielins by ectopic activation of the polyketide synthase 9 cluster in Fusarium graminearum.

AU - Sørensen, Jens Laurids

AU - Hansen, Frederik Teilfeldt

AU - Søndergaard, Teis

AU - Staerk, Dan

AU - V. Lee, Tet

AU - Wimmer, Reinhard

AU - G. Klitgaard, Louise

AU - Purup, Stig

AU - Giese, Henriette

AU - John Nordmand Frandsen, Rasmus

PY - 2012/5

Y1 - 2012/5

N2 - Like many other filamentous fungi, Fusarium graminearum has the genetic potential to produce a vast array of unknown secondary metabolites. A promising approach to determine the nature of these is to activate silent secondary metabolite gene clusters through constitutive expression of cluster specific transcription factors. We have developed a system in which an expression cassette containing the transcription factor from the targeted PKS cluster disrupts the production of the red mycelium pigment aurofusarin. This aids with identification of mutants as they appear as white colonies and metabolite analyses where aurofusarin and its intermediates are normally among the most abundant compounds. The system was used for constitutive expression of the local transcription factor from the PKS9 cluster (renamed FSL) leading to production of three novel fusarielins, F, G and H. This group of compounds has not previously been reported from F. graminearum or linked to a biosynthetic gene in any fungal species. The toxicity of the three novel fusarielins was examined against colorectal cancer cell lines where fusarielin H was more potent than fusarielin F and G.

AB - Like many other filamentous fungi, Fusarium graminearum has the genetic potential to produce a vast array of unknown secondary metabolites. A promising approach to determine the nature of these is to activate silent secondary metabolite gene clusters through constitutive expression of cluster specific transcription factors. We have developed a system in which an expression cassette containing the transcription factor from the targeted PKS cluster disrupts the production of the red mycelium pigment aurofusarin. This aids with identification of mutants as they appear as white colonies and metabolite analyses where aurofusarin and its intermediates are normally among the most abundant compounds. The system was used for constitutive expression of the local transcription factor from the PKS9 cluster (renamed FSL) leading to production of three novel fusarielins, F, G and H. This group of compounds has not previously been reported from F. graminearum or linked to a biosynthetic gene in any fungal species. The toxicity of the three novel fusarielins was examined against colorectal cancer cell lines where fusarielin H was more potent than fusarielin F and G.

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