白色链霉菌
基因簇
粘粒
异源表达
链霉菌
生物合成
生物
聚酮
异源的
生物化学
基因
遗传学
细菌
重组DNA
作者
Xiaohui Yan,Katharina Probst,Anton Linnenbrink,Moritz Arnold,Thomas Paululat,Axel Zeeck,Andreas Bechthold
出处
期刊:ChemBioChem
[Wiley]
日期:2011-12-12
卷期号:13 (2): 224-230
被引量:35
标识
DOI:10.1002/cbic.201100574
摘要
Abstract Mensacarcin is a potent cytotoxic agent isolated from Streptomyces bottropensis. It possesses a high content of oxygen atoms and two epoxide groups, and shows cytostatic and cytotoxic activity comparable to that of doxorubicin, a widely used drug for antitumor therapy. Another natural compound, rishirilide A, was also isolated from the fermentation broth of S. bottropensis . Screening a cosmid library of S. bottropensis with minimal PKS‐gene‐specific primers revealed the presence of three different type II polyketide synthase (PKS) gene clusters in this strain: the msn cluster (mensacarcin biosynthesis), the rsl cluster (rishirilide biosynthesis), and the mec cluster (putative spore pigment biosynthesis). Interestingly, luciferase‐like oxygenases, which are very rare in Streptomyces species, are enriched in both the msn cluster and the rsl cluster. Three cosmids, cos2 (containing the major part of the msn cluster), cos3 (harboring the mec cluster), and cos4 (spanning probably the whole rsl cluster) were introduced into the general heterologous host Streptomyces albus by intergeneric conjugation. Expression of cos2 and cos4 in S. albus led to the production of didesmethylmensacarcin (DDMM, a precursor of mensacarcin) and the production of rishirilide A and B (a precursor of rishirilide A), respectively. However, no product was detected from the expression of cos3. In addition, based on the results of isotope‐feeding experiments in S. bottropensis , a putative biosynthesis pathway for mensacarcin is proposed.
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