In Vitro Biosynthesis of the Core Scaffold of the Thiopeptide Thiomuracin

Hudson, Graham A.; Zhang, Zhengan; Tietz, Jonathan I.; Mitchell, Douglas A.; Donk, Wilfred A. van der

doi:10.1021/jacs.5b10194

Cited by 150 publications

(284 citation statements)

References 27 publications

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“…S5). A similar pattern of multiple glutamylations has previously been observed for nonthiopeptide RiPP pathways (22,25); however, in the in vitro reconstituted thiomuracin system, only a monoglutamylated intermediate accumulates when the TclL ortholog (TbtC) is omitted (11). This discrepancy may be due to the different reaction conditions (in vitro versus in vivo) or to an intrinsic difference in how this two-step dehydration process is coordinated in the two biosynthetic systems.…”

Section: Tclp Mediates the Transition Between Two Phases Of Core-peptidesupporting

confidence: 66%

“…Previous studies showed only MP1 is produced from the full set of genes, whereas only MP2 is formed in the ΔTclS strain (13). the recent in vitro thiomuracin study (11), may initiate processing. Indeed, the TclE peptide remains unmodified in the TclJ-defective strain (Fig.…”

Section: Tclp Mediates the Transition Between Two Phases Of Core-peptidementioning

confidence: 95%

“…These studies succeed in identifying extractable products and intermediates that have been prematurely cleaved from the leader peptide, but overlook peptide intermediates that are chemically very different from product molecules. In vitro studies of thiopeptide biosynthetic components have provided information about functional sets of enzymatic processing (11,12), but complete reconstitution remains a challenging endeavor. As an alternative approach, we recently reported an in vivo heterologous expression system that allows both efficient genetic changes in the core and biosynthetic enzymes and isolation and characterization of biochemical intermediates in micrococcin biosynthesis (13).…”

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confidence: 99%

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Capture of micrococcin biosynthetic intermediates reveals C-terminal processing as an obligatory step for in vivo maturation

Bewley

Bennallack

Burlingame

et al. 2016

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

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Thiopeptides, including micrococcins, are a growing family of bioactive natural products that are ribosomally synthesized and heavily modified. Here we use a refactored, modular in vivo system containing the micrococcin P1 (MP1) biosynthetic genes (TclIJKLMNPS) from Macrococcus caseolyticus str 115 in a genetically tractable Bacillus subtilis strain to parse the processing steps of this pathway. By fusing the micrococcin precursor peptide to an affinity tag and coupling it with catalytically defective enzymes, biosynthetic intermediates were easily captured for analysis. We found that two major phases of molecular maturation are separated by a key C-terminal processing step. Phase-I conversion of six Cys residues to thiazoles (TclIJN) is followed by C-terminal oxidative decarboxylation (TclP). This TclP-mediated oxidative decarboxylation is a required step for the peptide to progress to phase II. In phase II, Ser/Thr dehydration (TclKL) and peptide macrocycle formation (TclM) occurs. A C-terminal reductase, TclS, can optionally act on the substrate peptide, yielding MP1, and is shown to act late in the pathway. This comprehensive characterization of the MP1 pathway prepares the way for future engineering efforts.thiopeptide | affinity-tagged intermediates | biosynthesis | antibiotic | RiPP

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Section: Tclp Mediates the Transition Between Two Phases Of Core-peptidesupporting

confidence: 66%

Section: Tclp Mediates the Transition Between Two Phases Of Core-peptidementioning

confidence: 95%

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confidence: 99%

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Capture of micrococcin biosynthetic intermediates reveals C-terminal processing as an obligatory step for in vivo maturation

Bewley

Bennallack

Burlingame

et al. 2016

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

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“…For a typical thiopeptide gene cluster in nature, one often encounters numerous additional genes that obscure the simplicity of central thiopeptide chemistry. The recent in vitro reconstitution of the thiomuracin biosynthetic pathway illustrates this simplicity (17). In that study, five different protein enzymes, along with an additional RiPP precursor peptide recognition element (RRE)-containing protein, were found to be sufficient for the synthesis of a bioactive thiopeptide scaffold.…”

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confidence: 99%

“…In 2009, multiple independent researchers reported this general scheme for thiopeptide synthesis (11)(12)(13)(14)(15). In the years since, several additional biosynthetic principles have been elucidated (16)(17)(18). The process appears to involve three core steps: (i) cyclodehydration/oxidation of Cys residues to form thiazole heterocycles (Ser and Thr residues may also be modified to oxazoline or oxazole), (ii) dehydration of Ser and Thr residues yielding dehydroalanines and dehydrobutyrines, respectively, and (iii) cycloaddition of two of the dehydrated residues to yield the final macrocyclic thiopeptide scaffold (Fig.…”

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confidence: 99%

Reconstitution and Minimization of a Micrococcin Biosynthetic Pathway in Bacillus subtilis

et al. 2016

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Thiopeptides represent one of several families of highly modified peptide antibiotics that hold great promise for natural product engineering. These macrocyclic peptides are produced by a combination of ribosomal synthesis and extensive posttranslational modification by dedicated processing enzymes. We previously identified a compact, plasmid-borne gene cluster for the biosynthesis of micrococcin P1 (MP1), an archetypal thiopeptide antibiotic. In an effort to genetically dissect this pathway, we have reconstituted it in Bacillus subtilis. Successful MP1 production required promoter engineering and the reassembly of essential biosynthetic genes in a modular plasmid. The resulting system allows for rapid pathway manipulation, including protein tagging and gene deletion. We find that 8 processing proteins are sufficient for the production of MP1 and that the tailoring enzyme TclS catalyzes a C-terminal reduction step that distinguishes MP1 from its sister compound micrococcin P2. IMPORTANCEThe emergence of antibiotic resistance is one of the most urgent human health concerns of our day. A crucial component in an integrated strategy for countering antibiotic resistance is the ability to engineer pathways for the biosynthesis of natural and derivatized antimicrobial compounds. In this study, the model organism B. subtilis was employed to reconstitute and genetically modularize a 9-gene system for the biosynthesis of micrococcin, the founding member of a growing family of thiopeptide antibiotics.

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A Cell‐Free Platform Based on Nisin Biosynthesis for Discovering Novel Lanthipeptides and Guiding their Overproduction In Vivo

et al. 2020

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Lanthipeptides have extensive therapeutic and industrial applications. However, because many are bactericidal, traditional in vivo platforms are limited in their capacity to discover and mass produce novel lanthipeptides as bacterial organisms are often critical components in these systems. Herein, the development of a cell‐free protein synthesis (CFPS) platform that enables rapid genome mining, screening, and guided overproduction of lanthipeptides in vivo is described. For proof‐of‐concept studies, a type I lanthipeptide, nisin, is selected. Four novel lanthipeptides with antibacterial activity are identified among all nisin analogs in the National Center for Biotechnology Information (NCBI) database in a single day. Further, the CFPS platform is coupled with a screening assay for anti‐gram‐negative bacteria growth, resulting in the identification of a potent nisin mutant, M5. The titers of nisin and the nisin analog are found to be improved with CFPS platform guidance. Owing to the similarities in biosynthesis, the CFPS platform is broadly applicable to other lanthipeptides, thereby providing a universal method for lanthipeptide discovery and overproduction.

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In Vitro Biosynthesis of the Core Scaffold of the Thiopeptide Thiomuracin

Cited by 150 publications

References 27 publications

Capture of micrococcin biosynthetic intermediates reveals C-terminal processing as an obligatory step for in vivo maturation

Capture of micrococcin biosynthetic intermediates reveals C-terminal processing as an obligatory step for in vivo maturation

Reconstitution and Minimization of a Micrococcin Biosynthetic Pathway in Bacillus subtilis

A Cell‐Free Platform Based on Nisin Biosynthesis for Discovering Novel Lanthipeptides and Guiding their Overproduction In Vivo

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