Modulation of Polyketide Synthase Activity by Accessory Proteins During Lovastatin Biosynthesis

Kennedy, Jonathan; Auclair, Karine; Kendrew, Steven G.; Park, Cheonseok; Vederas, John C.; Hutchinson, C. Richard

doi:10.1126/science.284.5418.1368

Cited by 593 publications

(620 citation statements)

References 24 publications

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“…tatin is synthesized via the polyketide pathway [18,19]. After addition of lactose at 144 h of culture, a lovastatin specific generation rate of 0.242 mg (g biomass) −1 h −1 was obtained for the three C:N values tested.…”

Section: Resultsmentioning

confidence: 99%

Production of lovastatin by Aspergillus terreus: effects of the C:N ratio and the principal nutrients on growth and metabolite production

López

Pérez

Sevilla

et al. 2003

Enzyme and Microbial Technology

170

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Production of lovastatin and microbial biomass by Aspergillus terreus ATCC 20542 were influenced by the type of the carbon source (lactose, glycerol, and fructose) and the nitrogen source (yeast extract, corn steep liquor, and soybean meal) used and the C:N mass ratio in the medium. Use of a slowly metabolized carbon source (lactose) in combination with either soybean meal or yeast extract under N-limited conditions gave the highest titers and specific productivity (∼0.1 mg g −1 h −1 ) of lovastatin. The maximum value of the lovastatin yield coefficient on biomass was ∼30 mg g −1 using the lactose/soybean meal and lactose/yeast extract media. The optimal initial C:N mass ratio for attaining high productivity of lovastatin was ∼40. The behavior of the fermentation was not affected by the method of inoculation (fungal spores or hyphae) used, but the use of spores gave a more consistent inoculum in the different runs.

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Section: Resultsmentioning

confidence: 99%

Production of lovastatin by Aspergillus terreus: effects of the C:N ratio and the principal nutrients on growth and metabolite production

López

Pérez

Sevilla

et al. 2003

Enzyme and Microbial Technology

170

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“…In a noniterative modular PKS, each module is used only once, and the polyketide intermediate is transferred to a downstream module for chain elongation. The well-known anti-cholesterol natural product lovastatin is synthesized by two noniterative type I PKSs in Aspergillus terreus (2), whereas the antibiotic erythromycin is synthesized by a bacterial iterative type I PKS consisting of a loading module and six extension modules (3). Different from both of these is type II PKS, a large multienzyme complex of small, discrete enzymes with particular functions.…”

Section: Introductionmentioning

confidence: 99%

Type III polyketide synthases in natural product biosynthesis

et al. 2012

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SummaryPolyketides represent an important class of biologically active and structurally diverse compounds in nature. They are synthesized from acyl-coenzyme A substrates by polyketide synthases (PKSs). PKSs are classified into three groups: types I, II, and III. This article introduces recent studies on type III PKSs identified from plants, bacteria, and fungi, and describes the catalytic functions of these enzymes in detail. Plant type III PKSs have been widely studied, as exemplified by chalcone synthase, which plays an important role in the synthesis of plant metabolites. Bacterial type III PKSs fall into five groups, many of which were identified from Streptomyces, a genus that has been well known for its production of bioactive molecules and genetic alterability. Although it was believed that type III PKSs exist exclusively in plants and bacteria, recent fungal genome sequencing projects and biochemical studies revealed the presence of type III PKSs in filamentous fungi, which provides a new chance to study fungal secondary metabolism and synthesize ''unnatural'' natural products. Type III PKSs have been used for the biosynthesis of novel molecules through precursordirected and structure-based mutagenesis approaches.2012 IUBMB IUBMB Life, 64(4): [285][286][287][288][289][290][291][292][293][294][295] 2012

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“…Selective processing during two successive iterations of polyketide chain extension is a known feature in highly reducing fully iterative polyketide synthases 29, 30, 31. In the LovB PKS, for example, which synthesizes the nonaketide core of the cholesterol‐lowering compound lovastatin using a single PKS module, an integral methyltransferase domain selectively methylates the β‐ketothioester formed after three rounds of chain extension 29.…”

mentioning

confidence: 99%

“…In the LovB PKS, for example, which synthesizes the nonaketide core of the cholesterol‐lowering compound lovastatin using a single PKS module, an integral methyltransferase domain selectively methylates the β‐ketothioester formed after three rounds of chain extension 29. In vitro analysis of model thioester substrates for LovB has demonstrated that the methyltransferase is exquisitely specific for the tetraketide substrate, and that for this substrate, methylation effectively outcompetes prior ketoreduction 32.…”

mentioning

confidence: 99%

An Iterative Module in the Azalomycin F Polyketide Synthase Contains a Switchable Enoylreductase Domain

Zhai

Liu

et al. 2017

Angew Chem Int Ed

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Detailed analysis of the modular Type I polyketide synthase (PKS) involved in the biosynthesis of the marginolactone azalomycin F in mangrove Streptomyces sp. 211726 has shown that only nineteen extension modules are required to accomplish twenty cycles of polyketide chain elongation. Analysis of the products of a PKS mutant specifically inactivated in the dehydratase domain of extension‐module 1 showed that this module catalyzes two successive elongations with different outcomes. Strikingly, the enoylreductase domain of this module can apparently be “toggled” off and on : it functions in only the second of these two cycles. This novel mechanism expands our understanding of PKS assembly‐line catalysis and may explain examples of apparent non‐colinearity in other modular PKS systems.

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Modulation of Polyketide Synthase Activity by Accessory Proteins During Lovastatin Biosynthesis

Cited by 593 publications

References 24 publications

Production of lovastatin by Aspergillus terreus: effects of the C:N ratio and the principal nutrients on growth and metabolite production

Production of lovastatin by Aspergillus terreus: effects of the C:N ratio and the principal nutrients on growth and metabolite production

Type III polyketide synthases in natural product biosynthesis

An Iterative Module in the Azalomycin F Polyketide Synthase Contains a Switchable Enoylreductase Domain

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