Selective production of the itaconic acid-derived compounds 2-hydroxyparaconic and itatartaric acid

Selective production of the itaconic acid-derived compounds 2-hydroxyparaconic and itatartaric acid

There is a strong interest in itaconic acid in the medical and pharmaceutical sectors, both as an anti-bacterial compound and as an immunoregulator in mammalian macrophages. Fungal hosts also produce itaconic acid, and in addition they can produce two derivatives 2-hydroxyparaconic and itatartaric a...

Full description

Saved in:
Bibliographic Details
Main Authors: Philipp Ernst, Felicia Zlati, Larissa Kever, Astrid Wirtz, Rainer Goldbaum, Jörg Pietruszka, Benedikt Wynands, Julia Frunzke, Nick Wierckx
Format: Article
Language:English
Published: Elsevier 2024-12-01
Series:Metabolic Engineering Communications
Subjects:
Ustilago cynodontis
2-Hydroxyparaconic and itatartaric acid
Derivatives specificity
Metabolic engineering
Fermentation
Downstream processing
Online Access:http://www.sciencedirect.com/science/article/pii/S221403012400021X
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:There is a strong interest in itaconic acid in the medical and pharmaceutical sectors, both as an anti-bacterial compound and as an immunoregulator in mammalian macrophages. Fungal hosts also produce itaconic acid, and in addition they can produce two derivatives 2-hydroxyparaconic and itatartaric acid. Not much is known about these two derivatives, while their structural analogy to itaconate could open up several applications. In this study, we report the production of these two itaconate-derived compounds. By overexpressing the itaconate P450 monooxygenase Cyp3 in a previously engineered itaconate-overproducing Ustilago cynodontis strain, itaconate was converted to its lactone 2-hydroxyparaconate. The second product itatartarate is most likely the result of the subsequent lactone hydrolysis. A major challenge in the production of 2-hydroxyparaconate and itatartarate is their co-production with itaconate, leading to difficulties in their purification. Achieving high derivatives specificity was therefore the paramount objective. Different strategies were evaluated including process parameters such as substrate and pH, as well as strain engineering focusing on Cyp3 expression and product export. 2-hydroxyparaconate and itatartarate were successfully produced from glucose and glycerol, with the latter resulting in a higher derivatives specificity due to an overall slower metabolism on this non-preferred carbon source. The derivatives specificity could be further increased by metabolic engineering approaches including the exchange of the native itaconate transporter Itp1 with the Aspergillus terreus itaconate transporter MfsA. Both 2-hydroxyparaconate and itatartarate were recovered from fermentation supernatants following a pre-existing protocol. 2-hydroxyparaconate was recovered first through a process of evaporation, lactonization, and extraction with ethyl acetate. Subsequently, itatartarate could be obtained in the form of its sodium salt by saponification of the purified 2-hydroxyparaconate. Finally, several analytical methods were used to characterize the resulting products and their structures were confirmed by nuclear magnetic resonance spectroscopy. This work provides a promising foundation for obtaining 2-hydroxyparaconate and itatartarate in high purity and quantity. This will allow to unravel the full spectrum of potential applications of these novel compounds.
ISSN:2214-0301

Similar Items