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Construction of kanamycin B overproducing strain by genetic engineering of Streptomyces tenebrarius.

Authors :
Xianpu Ni
Li, Dan
Lihua Yang
Tingjiao Huang
Hao Li
Huanzhang Xia
Source :
Applied Microbiology & Biotechnology. Feb2011, Vol. 89 Issue 3, p723-731. 9p.
Publication Year :
2011

Abstract

Genetic engineering as an important approach to strain optimization has received wide recognition. Recent advances in the studies on the biosynthetic pathways and gene clusters of Streptomyces make stain optimization by genetic alteration possible. Kanamycin B is a key intermediate in the manufacture of the important medicines dibekacin and arbekacin, which belong to a class of antibiotics known as the aminoglycosides. Kanamycin could be prepared by carbamoylkanamycin B hydrolysis. However, carbamoylkanamycin B production in Streptomyces tenebrarius H6 is very low. Therefore, we tried to obtain high kanamycin B-producing strains that produced kanamycin B as a main component. In our work, aprD3 and aprD4 were clarified to be responsible for deoxygenation in apramycin and tobramycin biosynthesis. Based on this information, genes aprD3, aprQ (deduced apramycin biosynthetic gene), and aprD4 were disrupted to optimize the production of carbamoylkanamycin B. Compared with wild-type strain, mutant strain SPU313 (Δ aprD3, Δ aprQ, and Δ aprD4) produced carbamoylkanamycin B as a single antibiotic, whose production increased approximately fivefold. To construct a strain producing kanamycin B instead of carbamoylkanamycin B, the carbamoyl-transfer gene tacA was inactivated in strain SPU313. Mutant strain SPU314 (Δ aprD3, Δ aprQ, Δ aprD4, and Δ tacA) specifically produced kanamycin B, which was proven by LC-MS. This work demonstrated careful genetic engineering could significantly improve production and eliminate undesired products. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
01757598
Volume :
89
Issue :
3
Database :
Academic Search Index
Journal :
Applied Microbiology & Biotechnology
Publication Type :
Academic Journal
Accession number :
57407174
Full Text :
https://doi.org/10.1007/s00253-010-2908-5