Publications by authors named "Aileen R Lee"
Borosins are ribosomally synthesized and post-translationally modified peptides (RiPPs) containing backbone α--methylations. These modifications confer favorable pharmacokinetic properties including increased membrane permeability and resistance to proteolytic degradation. Previous studies have biochemically and bioinformatically explored several borosins, revealing (1) numerous domain architectures and (2) diverse core regions lacking conserved sequence elements.
View Article and Find Full Text PDFBorosins are ribosomally synthesized and post-translationally modified peptides containing backbone α- -methylations. Identification of borosin precursor peptides is difficult because (1) there are no conserved sequence elements among borosin precursor peptides and (2) the biosynthetic gene clusters contain numerous domain architectures and peptide fusions. To tackle this problem, we updated the genome mining tool RODEO to automatically evaluate putative borosin BGCs and identify precursor peptides.
View Article and Find Full Text PDFArticle Synopsis
- Biosynthetic gene clusters (BGCs) in microbes are important for producing secondary metabolites (SMs) that influence interactions within microbial communities and with hosts.
- Existing methods to identify BGCs from metagenomic data have limitations, including high computational demands, a narrow focus on BGC types, and lack of information about the resulting SMs.
- The newly developed tool, TaxiBGC, improves the prediction of BGCs by using taxonomy-guided methods, demonstrating better accuracy in simulated tests and revealing associations between BGCs/SMs and various human diseases in large metagenomic datasets.
Borosins are ribosomally synthesized and post-translationally modified peptides (RiPPs) with α--methylations installed on the peptide backbone that impart unique properties like proteolytic stability to these natural products. The borosin RiPP family was initially reported only in fungi until our recent discovery and characterization of a Type IV split borosin system in the metal-respiring bacterium . Here, we used hidden Markov models and sequence similarity networks to identify over 1600 putative pathways that show split borosin biosynthetic gene clusters are widespread in bacteria.
View Article and Find Full Text PDFBackbone N-methylations impart several favorable characteristics to peptides including increased proteolytic stability and membrane permeability. Nonetheless, amide bond N-methylations incorporated as post-translational modifications are scarce in nature and were first demonstrated in 2017 for a single set of fungal metabolites. Here we expand on our previous discovery of iterative, autocatalytic α- N-methylating precursor proteins in the borosin family of ribosomally encoded peptide natural products.
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