Properties of Multidrug-Resistant Mutants Derived from Heterologous Expression Chassis Strain Streptomyces albidoflavus J1074

Author:

Dolya Borys1,Hryhorieva Olena1,Sorochynska Khrystyna1,Lopatniuk Maria2,Ostash Iryna1,Tseduliak Vasylyna-Marta1ORCID,Sterndorff Eva Baggesgaard3,Jørgensen Tue Sparholt3,Gren Tetiana3,Dacyuk Yuriy4,Weber Tilmann3ORCID,Luzhetskyy Andriy2,Fedorenko Victor1,Ostash Bohdan1ORCID

Affiliation:

1. Department of Genetics and Biotechnology, Ivan Franko National University of Lviv, 79005 Lviv, Ukraine

2. Department of Pharmacy, Saarland University, 66123 Saarbrucken, Germany

3. The Novo Nordisk Foundation Center for Biosustainability, Technical University of Denmark, Kemitorvet, 2800 Kongens Lyngby, Denmark

4. Department of Mineral Geology and Geophysics, Ivan Franko National University of Lviv, 79005 Lviv, Ukraine

Abstract

Streptomyces albidoflavus J1074 is a popular platform to discover novel natural products via the expression of heterologous biosynthetic gene clusters (BGCs). There is keen interest in improving the ability of this platform to overexpress BGCs and, consequently, enable the purification of specialized metabolites. Mutations within gene rpoB for the β-subunit of RNA polymerase are known to increase rifampicin resistance and augment the metabolic capabilities of streptomycetes. Yet, the effects of rpoB mutations on J1074 remained unstudied, and we decided to address this issue. A target collection of strains that we studied carried spontaneous rpoB mutations introduced in the background of the other drug resistance mutations. The antibiotic resistance spectra, growth, and specialized metabolism of the resulting mutants were interrogated using a set of microbiological and analytical approaches. We isolated 14 different rpoB mutants showing various degrees of rifampicin resistance; one of them (S433W) was isolated for the first time in actinomycetes. The rpoB mutations had a major effect on antibiotic production by J1074, as evident from bioassays and LC-MS data. Our data support the idea that rpoB mutations are useful tools to enhance the ability of J1074 to produce specialized metabolites.

Funder

Ministry of Education and Science of Ukraine

National Research Fund of Ukraine

Novo Nordisk Foundation

Publisher

MDPI AG

Subject

Virology,Microbiology (medical),Microbiology

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