Preparation of erythromycin analogs having functional groups at C-15

被引：19

作者：

Ashley, Gary W.

Burlingame, Mark

Desai, Ruchir

Fu, Hong

Leaf, Tim

Licari, Peter J.

Tran, Chau

Abbanat, Darren

Bush, Karen

Macielag, Mark

机构：

[1] Kosan Biosci Inc, Hayward, CA 94545 USA

[2] Johnson & Johnson Pharmaceut Res & Dev LLC, Raritan, NJ 08869 USA

来源：

JOURNAL OF ANTIBIOTICS | 2006年 / 59卷 / 07期

关键词：

erythromycin; fluorine; azide; antibacterial; genetic engineering; polyketide;

D O I：

10.1038/ja.2006.56

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：

Chemobiosynthesis has been used to prepare analogs of erythromycins having unique functional groups at the 15-position. Using diketide thioester feeding to genetically engineered Streptomyces coelicolor, analogs of 6-deoxyerythronolide B were prepared having 15-fluoro, 15-chloro, and 15-azido groups. Bioconversion using a genetically engineered mutant of Saccharopolyspora erythraea was used to produce 15-fluoroerythromycin A and 15-azidoerythromycin A. These new erythromycin analogs provide antibacterial macrolides with unique physicochemical properties and functional groups that allow for selective derivatization.

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页码：392 / 401

页数：10

相关论文

共 15 条

[1] HYDROXYLATION AND N-DEMETHYLATION OF CLARITHROMYCIN (6-O-METHYLERYTHROMYCIN-A) BY MUCOR-CIRCINELLOIDES [J].

ADACHI, T ;

SASAKI, J ;

OMURA, S .

JOURNAL OF ANTIBIOTICS, 1989, 42 (09) :1433-1437

[2]

[Anonymous], [No title captured]

[3] PHARMACOKINETICS AND HUMAN-TISSUE PENETRATION OF FLURITHROMYCIN [J].

BENONI, G ;

CUZZOLIN, L ;

LEONE, R ;

CONSOLO, U ;

FERRONATO, G ;

BERTRAND, C ;

PUCHETTI, V ;

FRACASSO, ME .

ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1988, 32 (12) :1875-1878

[4] Fluorine in medicinal chemistry [J].

Böhm, HJ ;

Banner, D ;

Bendels, S ;

Kansy, M ;

Kuhn, B ;

Müller, K ;

Obst-Sander, U ;

Stahl, M .

CHEMBIOCHEM, 2004, 5 (05) :637-643

[5] Production of 6-deoxy-13-cyclopropyl-erythromycin B by Saccharopolyspora erythraea NRRL 18643 [J].

Brown, MS ;

Dirlam, JP ;

McArthur, HAI ;

McCormick, EL ;

Morse, BK ;

Murphy, PA ;

O'Connell, TN ;

Pacey, M ;

Rescek, DM ;

Ruddock, J ;

Wax, RG .

JOURNAL OF ANTIBIOTICS, 1999, 52 (08) :742-747

[6] N-Acyl-2-benzoxazolinones in titanium-mediated Aldol reactions [J].

Burlingame, MA ;

Mendoza, E ;

Ashley, GW .

TETRAHEDRON LETTERS, 2004, 45 (14) :2961-2964

[7] Saccharopolyspora erythraea-catalyzed bioconversion of 6-deoxyerythronolide B analogs for production of novel erythromycins [J].

Carreras, C ;

Frykman, S ;

Ou, S ;

Cadapan, L ;

Zavala, S ;

Woo, E ;

Leaf, T ;

Carney, J ;

Burlingame, M ;

Patel, S ;

Ashley, G ;

Licari, P .

JOURNAL OF BIOTECHNOLOGY, 2002, 92 (03) :217-228

[8] ACID-CATALYSED DECOMPOSITION OF SOME BETA-AZIDO-CARBONYL COMPOUNDS [J].

DAVIES, AJ ;

DONALD, ASR ;

MARKS, RE .

JOURNAL OF THE CHEMICAL SOCIETY C-ORGANIC, 1967, (21) :2109-&

[9] Precursor-directed production of erythromycin analogs by Saccharopolyspora erythraea [J].

Frykman, S ;

Leaf, T ;

Carreras, C ;

Licari, P .

BIOTECHNOLOGY AND BIOENGINEERING, 2001, 76 (04) :303-310

[10] Precursor-directed biosynthesis of erythromycin analogs by an engineered polyketide synthase [J].

Jacobsen, JR ;

Hutchinson, CR ;

Cane, DE ;

Khosla, C .

SCIENCE, 1997, 277 (5324) :367-369