Assessing the Flexibility of the Prochlorosin 2.8 Scaffold for Bioengineering Applications

Hegemann, Julian D.; Bobeica, Silvia C.; Walker, Mark C.; Bothwell, Ian R.; Donk, Wilfred A. van der

doi:10.1021/acssynbio.9b00080

Cited by 35 publications

(50 citation statements)

References 78 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Intriguingly, although their core peptide sequences are highly diverse, there are some hints that they are not random. For instance, engineering studies have shown that the substrate tolerance of ProcM is not limitless and that unlike the natural substrates that have been investigated, which generally make single ring patterns, non-natural substrates in which the positions of Ser/Cys are altered often lead to incomplete cyclization [109]. These observations suggest that despite their diversity, the core peptides in the genomes may have undergone selection to be good substrates for ProcM.…”

Section: How Might Prochlorosin Biosynthetic Pathways Have Evolved?mentioning

confidence: 99%

Mechanisms and Evolution of Diversity-Generating RiPP Biosynthesis

Donk

2021

Trends in Chemistry

Self Cite

View full text Add to dashboard Cite

Section: How Might Prochlorosin Biosynthetic Pathways Have Evolved?mentioning

confidence: 99%

Mechanisms and Evolution of Diversity-Generating RiPP Biosynthesis

Donk

2021

Trends in Chemistry

Self Cite

View full text Add to dashboard Cite

“…These studies resulted in the discovery of lanthipeptide inhibitors of HIV budding process, 15 urokinase plasminogen activator 16 and α v β 3 integrin binders. 13 Similarly, we anticipate that the integration of the FIT-Laz system with powerful in vitro screening techniques such as mRNA display 66 will provide access to artificial thiopeptides with desirable pharmacological profiles for drug discovery purposes.…”

Section: Discussionmentioning

confidence: 99%

Minimal lactazole scaffold for in vitro production of pseudo-natural thiopeptides

Vinogradov

Shimomura

Ozaki

et al. 2019

Preprint

View full text Add to dashboard Cite

26Lactazole A is a cryptic thiopeptide from Streptomyces lactacystinaeus, encoded by a compact 9.8 kb 27 biosynthetic gene cluster. Here, we established a platform for in vitro biosynthesis of lactazole A, 28 referred to as the FIT -Laz system, via a combination of the flexible in vitro translation (FIT) system 29 with recombinantly produced lactazole biosynthetic enzymes. Systematic dissection of lactazole 30 biosynthesis revealed remarkable substrate tolerance of the biosynthetic enzymes, and led to the 31 development of the "minimal lactazole scaffold", a construct requiring only 6 post-translational 32 modifications for macrocyclization. Efficient assembly of such minimal thiopeptides with FIT-Laz 33 enabled access to diverse lactazole analogs with 10 consecutive mutations, 14-to 62-membered 34 macrocycles, and up to 18 amino acid-long tail regions. Moreover, utilizing genetic code 35 reprogramming, we demonstrated synthesis of pseudo-natural lactazoles containing 4 non-36 proteinogenic amino acids. This work opens possibilities in exploring novel sequence space of pseudo-37 natural thiopeptides. 38 39 595

show abstract

“…Eine dieser Varianten zeigte ebenfalls eine hohe Bindungsaffi nität zu dem αvβ3-Integrin (Abb. 2E, [9]).…”

Section: Das Lanthipeptid Prochlorosin 28unclassified

“…Durch die Nutzung degenerierter Oligonukleotid-Primer konnte eine Bibliothek aus etwa 10 6 verschiedenen Prochlorosin-2.8-Varianten erzeugt werden [10]. Durch Screening dieser Bibliothek konnte ein Inhibitor der Protein-Protein-Interaktion zwischen dem HIV-p6-Protein und der UEV-Domäne des humanen Proteins TSG101 identifi ziert werden [9]. Diese Wechselwirkung ist essenziell für die Knospung von HIV-Partikeln in infi zierten Zellen.…”

Section: Das Lanthipeptid Prochlorosin 28unclassified

Das Potenzial von RiPPs in medizinisch-biotechnologischen Anwendungen

Hegemann

2020

Biospektrum

Self Cite

View full text Add to dashboard Cite

Ribosomally synthesized and post-translationally modified proteins (RiPPs) are an interesting natural product superfamily. Their underlying biosynthetic principles, where recognition sites are strictly separated from the regions that are modified in the substrate, make them interesting for utilization in medicinal and biotechnological applications. Here, the promiscuity of RiPP biosynthetic enzymes will be described for examples from the lasso and lanthipeptide subfamilies and current developments as well as future directions in this field will be discussed.

show abstract

Assessing the Flexibility of the Prochlorosin 2.8 Scaffold for Bioengineering Applications

Cited by 35 publications

References 78 publications

Mechanisms and Evolution of Diversity-Generating RiPP Biosynthesis

Mechanisms and Evolution of Diversity-Generating RiPP Biosynthesis

Minimal lactazole scaffold for in vitro production of pseudo-natural thiopeptides

Das Potenzial von RiPPs in medizinisch-biotechnologischen Anwendungen

Contact Info

Product

Resources

About