MUTANTS OF A LOVASTATIN-HYPERPRODUCING ASPERGILLUS-TERREUS DEFICIENT IN THE PRODUCTION OF SULOCHRIN

被引：45

作者：

VINCI, VA ^{[1
]}

HOERNER, TD ^{[1
]}

COFFMAN, AD ^{[1
]}

SCHIMMEL, TG ^{[1
]}

DABORA, RL ^{[1
]}

KIRPEKAR, AC ^{[1
]}

RUBY, CL ^{[1
]}

STIEBER, RW ^{[1
]}

机构：

[1] MERCK & CO INC,MSDRL,RAHWAY,NJ 07065

来源：

JOURNAL OF INDUSTRIAL MICROBIOLOGY | 1991年 / 8卷 / 02期

关键词：

MICROTITER FERMENTATION; LOVASTATIN; POLYKETIDE; STRAIN IMPROVEMENT; SCREENING;

D O I：

10.1007/BF01578762

中图分类号：

Q81 [生物工程学（生物技术）]; Q93 [微生物学];

学科分类号：

071005 ; 0836 ; 090102 ; 100705 ;

摘要：

A lovastatin-hyperproducing culture of Aspergillus terreus was shown to produce several co-metabolites extracted from whole broth. The predominant co-metabolite was the benzophenone, sulochrin, reported to arise from a polyketide biosynthetic pathway. This compound was targeted for elimination by classical mutagenesis and screening. A surface culture method employing microtiter plates was used to ferment mutants for the primary screen. Qualitative determinations of lovastatin and sulochrin production were achieved by high-performance thin-layer chromatography. A mutant, strain AH6, which produced lovastatin titers equivalent to the parent culture and no detectable sulochrin was isolated. In addition, a lovastatin-hyperproducing mutant designated CB4 was capable of producing 16% more lovastatin and 30% less sulochrin than the parent culture in shake flask fermentations. In a pilot-scale 250-gallon fermentation, strain CB4 gave a 20% increase in lovastatin titer while producing 83% less sulochrin than the parent culture.

引用

页码：113 / 120

页数：8

共 18 条

[1] MEVINOLIN - A HIGHLY POTENT COMPETITIVE INHIBITOR OF HYDROXYMETHYLGLUTARYL-COENZYME-A REDUCTASE AND A CHOLESTEROL-LOWERING AGENT [J].

ALBERTS, AW ;

CHEN, J ;

KURON, G ;

HUNT, V ;

HUFF, J ;

HOFFMAN, C ;

ROTHROCK, J ;

LOPEZ, M ;

JOSHUA, H ;

HARRIS, E ;

PATCHETT, A ;

MONAGHAN, R ;

CURRIE, S ;

STAPLEY, E ;

ALBERSSCHONBERG, G ;

HENSENS, O ;

HIRSHFIELD, J ;

HOOGSTEEN, K ;

LIESCH, J ;

SPRINGER, J .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1980, 77 (07) :3957-3961

[2]

Buckland B., 1989, NOVEL MICROB PROD ME, V70, P161, DOI [10.4103/0250-474X.49087, DOI 10.4103/0250-474X.49087]

[3]

CURTIS RF, 1960, THOM J CHEM SOC, P4836

[4] SCREENING AND MUTAGENESIS OF MOLDS FOR THE IMPROVEMENT OF GLUCOSE-OXIDASE PRODUCTION [J].

FIEDUREK, J ;

ROGALSKI, J ;

ILCZUK, Z ;

LEONOWICZ, A .

ENZYME AND MICROBIAL TECHNOLOGY, 1986, 8 (12) :734-736

[5]

FUJII I, 1982, CHEM PHARM BULL, V30, P2283

[6] NATURAL-PRODUCTS FROM FUNGI .25. BIOSYNTHESIS OF SECO-ANTHRAQUINONES GEODIN AND DIHYDROGEODIN FROM EMODIN [J].

FUJIMOTO, H ;

FLASCH, H ;

FRANCK, B .

CHEMISCHE BERICHTE-RECUEIL, 1975, 108 (04) :1224-1228

[7]

INAMORI Y, 1983, CHEM PHARM BULL, V31, P4543

[8]

KIRIYAMA N, 1977, CHEM PHARM BULL, V25, P2593

[9]

LEIN J, 1983, ASM NEWS, V12, P576

[10] HISTORY OF YIELD IMPROVEMENTS IN THE PRODUCTION OF ASPERLICIN BY ASPERGILLUS-ALLIACEUS [J].

MONAGHAN, RL ;

ARCURI, E ;

BAKER, EE ;

BUCKLAND, BC ;

GREASHAM, RL ;

HOUCK, DR ;

IHNEN, ED ;

INAMINE, ES ;

KING, JJ ;

LESNIAK, E ;

MASUREKAR, PS ;

SCHULMAN, CA ;

SINGLETON, B ;

GOETZ, MA .

JOURNAL OF INDUSTRIAL MICROBIOLOGY, 1989, 4 (02) :97-104

← 1 2 →