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Systems metabolic engineering of Corynebacterium glutamicum for the bioproduction of biliverdin via protoporphyrin independent pathway

Authors
Seok, JihoKo, Young JinLee, Myeong-EunHyeon, Jeong EunHan, Sung Ok
Issue Date
29-Mar-2019
Publisher
BMC
Keywords
Biliverdin; Corynebacterium glutamicum; In vitro thermodynamic analysis; Coproporphyrin dependent pathway; Synthetic biology; Metabolic engineering
Citation
JOURNAL OF BIOLOGICAL ENGINEERING, v.13
Indexed
SCIE
SCOPUS
Journal Title
JOURNAL OF BIOLOGICAL ENGINEERING
Volume
13
URI
https://scholar.korea.ac.kr/handle/2021.sw.korea/66593
DOI
10.1186/s13036-019-0156-5
ISSN
1754-1611
Abstract
BackgroundBiliverdin, a prospective recyclable antioxidant and one of the most important precursors for optogenetics, has received growing attention. Biliverdin is currently produced by oxidation of bilirubin from mammalian bile using chemicals. However, unsustainable procedures of extraction, chemical oxidation, and isomer separation have prompted bio-based production using a microbial cell factory.ResultsIn vitro thermodynamic analysis was performed to show potential candidates of bottleneck enzymes in the pathway to produce biliverdin. Among the candidates, hemA and hemL were overexpressed in Corynebacterium glutamicum to produce heme, precursor of biliverdin. To increase precursor supply, we suggested a novel hemQ-mediated coproporphyrin dependent pathway rather than noted hemN-mediated protoporphyrin dependent pathway in C. glutamicum. After securing precursors, hmuO was overexpressed to pull the carbon flow to produce biliverdin. Through modular optimization using gene rearrangements of hemA, hemL, hemQ, and hmuO, engineered C. glutamicum BV004 produced 11.380.47mg/L of biliverdin at flask scale. Fed-batch fermentations performed in 5L bioreactor with minimal medium using glucose as a sole carbon source resulted in the accumulation of 68.74 +/- 4.97mg/L of biliverdin, the highest titer to date to the best of our knowledge.Conclusions We developed an eco-friendly microbial cell factory to produce biliverdin using C. glutamicum as a biosystem. Moreover, we suggested that C. glutamicum has the thermodynamically favorable coproporphyrin dependent pathway. This study indicated that C. glutamicum can work as a powerful platform to produce biliverdin as well as heme-related products based on the rational design with in vitro thermodynamic analysis.
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