Abstract:<div>
<p>Engineering of nonribosomal peptide
synthetases (NRPS) has faced numerous obstacles despite being an attractive
path towards novel bioactive molecules. Specificity filters in the nonribosomal
peptide assembly line determine engineering success, but the relative contribution
of adenylation (A-) and condensation (C-)domains is under debate. In the engineered,
bimodular NRPS sdV-GrsA/GrsB1, the first module is a subdomain-swapped chimera
showing substrate promiscuity. On sdV-GrsA and evolved… Show more
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