The Neocarzinostatin Biosynthetic Gene Cluster from Streptomyces carzinostaticus ATCC 15944 Involving Two Iterative Type I Polyketide Synthases

Liu, Wen; Nonaka, Kazuhiro; Nie, Liping; Zhang, Jian; Christenson, Steven D.; Bae, Juyun; Lanen, Steven G. Van; Zazopoulos, Emmanuel; Farnet, Chris M.; Yang, Catherine F.; Shen, Ben

doi:10.1016/j.chembiol.2004.12.013

Cited by 119 publications

(135 citation statements)

References 25 publications

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“…In actinomycetes, this type of simple aromatic polyketides is generally biosynthesized by an iterative type I polyketide synthase (PKS) [15], which has been quite recently established and are encoded in the avilamycin [16], calicheamicin [17], neocarzinostatin [18], chlorothricin [19], biosynthetic gene clusters. Therefore, an iterative type I PKS was also anticipated to be involved in the biosynthesis of pactamycin.…”

Section: Introductionmentioning

confidence: 99%

Cloning of the Pactamycin Biosynthetic Gene Cluster and Characterization of a Crucial Glycosyltransferase Prior to a Unique Cyclopentane Ring Formation

et al. 2007

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The biosynthetic gene (pct) cluster for an antitumor antibiotic pactamycin was identified by use of a gene for putative radical S-adenosylmethionine methyltransferase as a probe. The pct gene cluster is localized to a 34 kb contiguous DNA from Streptomyces pactum NBRC 13433 and contains 24 open reading frames. Based on the bioinformatic analysis, a plausible biosynthetic pathway for pactamycin comprising of a unique cyclopentane ring, 3-aminoacetophenone, and 6-methylsalicylate was proposed. The pctL gene encoding a glycosyltransferase was speculated to be involved in an N-glycoside formation between 3-aminoacetophenone and UDP-N-acetyl-a -D-glucosamine prior to a unique cyclopentane ring formation. The pctL gene was then heterologously expressed in Escherichia coli and the enzymatic activity of the recombinant PctL protein was investigated. Consequently, the PctL protein was found to catalyze the expected reaction forming b-N-glycoside. The enzymatic activity of the PctL protein clearly confirmed that the present identified gene cluster is for the biosynthesis of pactamycin. Also, a glycosylation prior to cyclopentane ring formation was proposed to be a general strategy in the biosynthesis of the structurally related cyclopentane containing compounds.

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Section: Introductionmentioning

confidence: 99%

Cloning of the Pactamycin Biosynthetic Gene Cluster and Characterization of a Crucial Glycosyltransferase Prior to a Unique Cyclopentane Ring Formation

et al. 2007

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“…We finally wished to extend the findings for SgcE and NcsE to demonstrate that all PKSE are likely functionally equivalent, thereby solidifying a common mechanism for initiation of enediyne biosynthesis. This was accomplished by plasmid-based expression of heterologous PKSE gene cassettes within two Streptomyces hosts: SB1005 and SB5002, ⌬sgcE and ⌬ncsE mutant strains devoid of C-1027 and NCS production, respectively (13,14). Plasmids pBS1049, pBS5020 (14), and pBS10005 (15), which contain sgcE, ncsE, and mdpE (the PKSE gene from the MDP cluster), respectively, were prepared and introduced into SB1005 by conjugation.…”

Section: Acp Domain Is Posttranslationally Modified By a C-terminal Pmentioning

confidence: 99%

“…This was accomplished by plasmid-based expression of heterologous PKSE gene cassettes within two Streptomyces hosts: SB1005 and SB5002, ⌬sgcE and ⌬ncsE mutant strains devoid of C-1027 and NCS production, respectively (13,14). Plasmids pBS1049, pBS5020 (14), and pBS10005 (15), which contain sgcE, ncsE, and mdpE (the PKSE gene from the MDP cluster), respectively, were prepared and introduced into SB1005 by conjugation. Using HPLC and matrix-assisted laser-desorption ionization-MS to monitor production, all of the recombinant strains gave [MϩH] ϩ ions at m/z ϭ 844.259 and 846.272, consistent with the molecular formula for C-1027 and its aromatized product and identical to those isolated from the wild-type strain (SI Table 3) (13).…”

Section: Acp Domain Is Posttranslationally Modified By a C-terminal Pmentioning

confidence: 99%

“…Inspired by the ability to map the ACP active site of recombinant SgcE, we prepared an E. coli expression plasmid for NcsE, the PKSE involved in NCS biosynthesis in Streptomyces carzinostaticus (14), and the protein was purified to near homogeneity (SI Fig. 6).…”

Section: Si Text)mentioning

confidence: 99%

“…The biosynthetic gene clusters for C-1027 (13), NCS (14), MDP (15), and CAL (16) have been cloned and sequenced, and the first biosynthetic step leading to the enediyne core was speculated to be catalyzed by a new type of iterative polyketide synthase (PKS) that is shared among the entire enediyne family (12)(13)(14)(15)(16). PKSs catalyze decarboxylative condensation similar to fatty acid synthases (FASs) and likewise share homologous ketosynthase (KS) domains, responsible for decarboxylation and condensation, and acyltransferase (AT) domains, responsible for selection and loading of an acyl CoA (CoA)-substrate to a free thiol of an acyl carrier protein (ACP).…”

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A phosphopantetheinylating polyketide synthase producing a linear polyene to initiate enediyne antitumor antibiotic biosynthesis

Zhang¹,

Lanen

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

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136

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The enediynes, unified by their unique molecular architecture and mode of action, represent some of the most potent anticancer drugs ever discovered. The biosynthesis of the enediyne core has been predicted to be initiated by a polyketide synthase (PKS) that is distinct from all known PKSs. Characterization of the enediyne PKS involved in C-1027 (SgcE) and neocarzinostatin (NcsE) biosynthesis has now revealed that (i) the PKSs contain a central acyl carrier protein domain and C-terminal phosphopantetheinyl transferase domain; (ii) the PKSs are functional in heterologous hosts, and coexpression with an enediyne thioesterase gene produces the first isolable compound, 1,3,5,7,9,11,13-pentadecaheptaene, in enediyne core biosynthesis; and (iii) the findings for SgcE and NcsE are likely shared among all nine-membered enediynes, thereby supporting a common mechanism to initiate enediyne biosynthesis.C-1027 ͉ neocarzinostatin ͉ phosphopantetheinyl transferase

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Combinatorial Biosynthesis of Pharmaceutical Natural Products

Liu

2009

Biocatalysis for the Pharmaceutical Industry

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The Neocarzinostatin Biosynthetic Gene Cluster from Streptomyces carzinostaticus ATCC 15944 Involving Two Iterative Type I Polyketide Synthases

Cited by 119 publications

References 25 publications

Cloning of the Pactamycin Biosynthetic Gene Cluster and Characterization of a Crucial Glycosyltransferase Prior to a Unique Cyclopentane Ring Formation

Cloning of the Pactamycin Biosynthetic Gene Cluster and Characterization of a Crucial Glycosyltransferase Prior to a Unique Cyclopentane Ring Formation

A phosphopantetheinylating polyketide synthase producing a linear polyene to initiate enediyne antitumor antibiotic biosynthesis

Combinatorial Biosynthesis of Pharmaceutical Natural Products

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