Understanding D-xylonic acid accumulation: a cornerstone for better metabolic engineering approaches.

Appl Microbiol Biotechnol

Environmental Waste Recycle Institute (EWRI), Department of Energy Science and Technology (DEST), Myongji University, Myongji-ro 116, Cheoin-gu, Yongin City, Gyeonggi Province, 17058, South Korea.

Published: July 2021

AI Article Synopsis

  • The xylose oxidative pathway (XOP) in engineered microorganisms is promising for producing various industrial compounds, but its efficiency is often limited by the toxic accumulation of D-xylonic acid, which affects cell growth and product formation.
  • Strategies to mitigate D-xylonic acid accumulation include genetic engineering methods that enhance enzyme expression and optimize metabolic pathways, focusing particularly on bacterial strains.
  • Understanding the causes of D-xylonic acid buildup is crucial for developing effective microbial cell factories, which can ultimately improve the production yields of valuable industrial products.

Article Abstract

The xylose oxidative pathway (XOP) has been engineered in microorganisms for the production of a wide range of industrially relevant compounds. However, the performance of metabolically engineered XOP-utilizing microorganisms is typically hindered by D-xylonic acid accumulation. It acidifies the media and perturbs cell growth due to toxicity, thus curtailing enzymatic activity and target product formation. Fortunately, from the growing portfolio of genetic tools, several strategies that can be adapted for the generation of efficient microbial cell factories have been implemented to address D-xylonic acid accumulation. This review centers its discussion on the causes of D-xylonic acid accumulation and how to address it through different engineering and synthetic biology techniques with emphasis given on bacterial strains. In the first part of this review, the ability of certain microorganisms to produce and tolerate D-xylonic acid is also tackled as an important aspect in developing efficient microbial cell factories. Overall, this review could shed some insights and clarity to those working on XOP in bacteria and its engineering for the development of industrially applicable product-specialist strains. KEY POINTS: D-Xylonic acid accumulation is attributed to the overexpression of xylose dehydrogenase concomitant with basal or inefficient expression of enzymes involved in D-xylonic acid assimilation. Redox imbalance and insufficient cofactors contribute to D-xylonic acid accumulation. Overcoming D-xylonic acid accumulation can increase product formation among engineered strains. Engineering strategies involving enzyme engineering, evolutionary engineering, coutilization of different sugar substrates, and synergy of different pathways could potentially address D-xylonic acid accumulation.

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Source
http://dx.doi.org/10.1007/s00253-021-11410-yDOI Listing

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