The mixed cultivation of Streptomyces sp. for doxorubicin production = 유사 생합성 경로를 가진 Streptomyces sp.의 혼합배양을 이용한 Doxorubicin 생합성

Abstract

We selected two mutants namely strain D5 and Nu23 by mutage- nesis of anthracycline producing Streptomyces: the former is an ε-rhodomycinone overproducing mutant selected from Streptomyces sp. C5, a baumycin producer and the latter, a blocked mutant of early pathway for doxorubicin biosynthesis obtained from Streptomyces peucetius ATCC 27952, a doxorubicin producer. The mutant strain Nu23 does not produce anthracycline metabolites but retains the most of enzyme activities converting aklavinone to doxorubicin and the mutant strain D5 produced ε-rhodomycinone at a level of 150 μg/ml. These strains were grown separately in NDYE medium and each was mixed at day 3 by equal volume of culture broth but the quantity of doxorubicin produced was far below an estimation based on the level of ε-rhodomycinone normaly produced by the strain D5. On the other hand doxorubicin was reached at maximum level after 4 days in the mixed culture condition which was composed of culture broth of strain D5 grown for 6 day and that of strain Nu23 grown for 3 day. It was turned out that the growth of mutant strain D5 was inhibited by the accumulation of daunorubicin and doxorubicin in mixed culture broth, which cause the limitation of ε-rhodomycinone.