Biosynthesis of Strained Amino Acids Through a PLP-Dependent Enzyme via Cryptic Halogenation

Author:

Sosa Max B.ORCID,Leeman Jacob T.,Washington Lorenzo J.ORCID,Scheller Henrik V.ORCID,Chang Michelle C. Y.

Abstract

AbstractAmino acids (AAs) are modular and modifiable building blocks which nature uses to synthesize both macromolecules, such as proteins, and small molecule natural products, such as alkaloids and non-ribosomal peptides (NRPs). While the 20 main proteinogenic AAs display relatively limited side-chain diversity, a wide range of non-canonical amino acids (ncAAs) exist that are not used by the ribosome for protein synthesis but contain a broad array of structural features and functional groups not found in proteinogenic AAs. In this communication, we report the discovery of the biosynthetic pathway for a new ncAA, pazamine, which contains a cyclopropane ring formed in two steps. In the first step, a chlorine is added onto the C4position of lysine by a radical halogenase PazA. The cyclopropane ring is then formed in the next step by a pyridoxal-5’-phosphate-dependent enzyme, PazB, via an SN2-like attack onto C4to eliminate chloride. Genetic studies of this pathway in the native host,Pseudomonas azotoformans, show that pazamine and its succinylated derivative, pazamide, potentially inhibit ethylene biosynthesis in growing plants based on alterations in the root phenotype ofArabidopsis thalianaseedlings. We further show that PazB can be utilized to make an alternative cyclobutane-containing AA. These discoveries may lead to advances in biocatalytic production of specialty chemicals and agricultural biotechnology.

Publisher

Cold Spring Harbor Laboratory

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