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Activation and enhancement of caerulomycin A biosynthesis in marine-derived Actinoalloteichus sp. AHMU CJ021 by combinatorial genome mining strategies.

Authors :
Xie, Yunchang
Chen, Jiawen
Wang, Bo
Chen, Tai
Chen, Junyu
Zhang, Yuan
Liu, Xiaoying
Chen, Qi
Source :
Microbial Cell Factories. 8/6/2020, Vol. 19 Issue 1, p1-14. 14p. 3 Diagrams, 2 Charts, 3 Graphs.
Publication Year :
2020

Abstract

Background: Activation of silent biosynthetic gene clusters (BGCs) in marine-derived actinomycete strains is a feasible strategy to discover bioactive natural products. Actinoalloteichus sp. AHMU CJ021, isolated from the seashore, was shown to contain an intact but silent caerulomycin A (CRM A) BGC-cam in its genome. Thus, a genome mining work was preformed to activate the strain's production of CRM A, an immunosuppressive drug lead with diverse bioactivities. Results: To well activate the expression of cam, ribosome engineering was adopted to treat the wild type Actinoalloteichus sp. AHMU CJ021. The initial mutant strain XC-11G with gentamycin resistance and CRM A production titer of 42.51 ± 4.22 mg/L was selected from all generated mutant strains by gene expression comparison of the essential biosynthetic gene-camE. The titer of CRM A production was then improved by two strain breeding methods via UV mutagenesis and cofactor engineering-directed increase of intracellular riboflavin, which finally generated the optimal mutant strain XC-11GUR with a CRM A production titer of 113.91 ± 7.58 mg/L. Subsequently, this titer of strain XC-11GUR was improved to 618.61 ± 16.29 mg/L through medium optimization together with further adjustment derived from response surface methodology. In terms of this 14.6 folds increase in the titer of CRM A compared to the initial value, strain XC-GUR could be a well alternative strain for CRM A development. Conclusions: Our results had constructed an ideal CRM A producer. More importantly, our efforts also had demonstrated the effectiveness of abovementioned combinatorial strategies, which is applicable to the genome mining of bioactive natural products from abundant actinomycetes strains. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
14752859
Volume :
19
Issue :
1
Database :
Academic Search Index
Journal :
Microbial Cell Factories
Publication Type :
Academic Journal
Accession number :
145029086
Full Text :
https://doi.org/10.1186/s12934-020-01418-w