Production of a novel polyketide through the construction of a hybrid polyketide synthase

被引：99

作者：

Kuhstoss, S

Huber, M

Turner, JR

Paschal, JW

Rao, RN

机构：

[1] Lilly Research Laboratories, Lilly Corporate Center, Indianapolis

来源：

GENE | 1996年 / 183卷 / 1-2期

关键词：

macrolide; platenolide; spiramycin; tylactone; tylosin; Streptomyces; gene fusion;

D O I：

10.1016/S0378-1119(96)00565-3

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

The lactone rings of the polyketides platenolide and tylactone are synthesized by condensation of acetate-, proprionate-, and butyrate-derived precursors. A hybrid tylactone/platenolide synthase was constructed to determine if the choice of substrate is programmed by the polyketide synthase and to ascertain if a substrate different than that normally used in the first step of platenolide synthesis could be incorporated into the final polyketide. In this work, we report the successful incorporation of a propionate in place of the acetate normally used in the first step of platenolide synthesis. This result demonstrates that polyketide synthases choose a particular substrate at defined steps and provides strong evidence that substrate choice is programmed by the acyl transferase domain of a large, multifunctional polyketide synthase.

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收藏

页码：231 / 236

页数：6

相关论文

共 35 条

[1] SINGLE-STRANDED HEXAMERIC LINKERS - A SYSTEM FOR IN-PHASE INSERTION MUTAGENESIS AND PROTEIN ENGINEERING [J].

BARANY, F .

GENE, 1985, 37 (1-3) :111-123

[2] A MUTANT GENERATED BY EXPRESSION OF AN ENGINEERED DEBS1 PROTEIN FROM THE ERYTHROMYCIN-PRODUCING POLYKETIDE SYNTHASE (PKS) IN STREPTOMYCES-COELICOLOR PRODUCES THE TRIKETIDE AS A LACTONE, BUT THE MAJOR PRODUCT IS THE NOR-ANALOG DERIVED FROM ACETATE AS STARTER ACID [J].

BROWN, MJB ;

CORTES, J ;

CUTTER, AL ;

LEADLAY, PF ;

STAUNTON, J .

JOURNAL OF THE CHEMICAL SOCIETY-CHEMICAL COMMUNICATIONS, 1995, (15) :1517-1518

[3] AN UNUSUALLY LARGE MULTIFUNCTIONAL POLYPEPTIDE IN THE ERYTHROMYCIN-PRODUCING POLYKETIDE SYNTHASE OF SACCHAROPOLYSPORA-ERYTHRAEA [J].

CORTES, J ;

HAYDOCK, SF ;

ROBERTS, GA ;

BEVITT, DJ ;

LEADLAY, PF .

NATURE, 1990, 348 (6297) :176-178

[4] REPOSITIONING OF A DOMAIN IN A MODULAR POLYKETIDE SYNTHASE TO PROMOTE SPECIFIC CHAIN CLEAVAGE [J].

CORTES, J ;

WIESMANN, KEH ;

ROBERTS, GA ;

BROWN, MJB ;

STAUNTON, J ;

LEADLAY, PF .

SCIENCE, 1995, 268 (5216) :1487-1489

[5] A COMPREHENSIVE SET OF SEQUENCE-ANALYSIS PROGRAMS FOR THE VAX [J].

DEVEREUX, J ;

HAEBERLI, P ;

SMITHIES, O .

NUCLEIC ACIDS RESEARCH, 1984, 12 (01) :387-395

[6] ORGANIZATION OF THE ENZYMATIC DOMAINS IN THE MULTIFUNCTIONAL POLYKETIDE SYNTHASE INVOLVED IN ERYTHROMYCIN FORMATION IN SACCHAROPOLYSPORA-ERYTHRAEA [J].

DONADIO, S ;

KATZ, L .

GENE, 1992, 111 (01) :51-60

[7] AN ERYTHROMYCIN ANALOG PRODUCED BY REPROGRAMMING OF POLYKETIDE SYNTHESIS [J].

DONADIO, S ;

MCALPINE, JB ;

SHELDON, PJ ;

JACKSON, M ;

KATZ, L .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1993, 90 (15) :7119-7123

[8] MODULAR ORGANIZATION OF GENES REQUIRED FOR COMPLEX POLYKETIDE BIOSYNTHESIS [J].

DONADIO, S ;

STAVER, MJ ;

MCALPINE, JB ;

SWANSON, SJ ;

KATZ, L .

SCIENCE, 1991, 252 (5006) :675-679

[9] STUDIES ON BIOSYNTHESIS OF BASIC 16-MEMBERED MACROLIDE ANTIBIOTICS, PLATENOMYCINS .3. PRODUCTION, ISOLATION AND STRUCTURES OF PLATENOLIDES-I AND PLATENOLIDES-II [J].

FURUMAI, T ;

SUZUKI, M .

JOURNAL OF ANTIBIOTICS, 1975, 28 (10) :783-788

[10] CHARACTERIZATION OF A NOVEL REGULATORY GENE GOVERNING THE EXPRESSION OF A POLYKETIDE SYNTHASE GENE IN STREPTOMYCES-AMBOFACIENS [J].

GEISTLICH, M ;

LOSICK, R ;

TURNER, JR ;

RAO, RN .

MOLECULAR MICROBIOLOGY, 1992, 6 (14) :2019-2029

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