POSTTRANSLATIONAL MODIFICATIONS IN MICROCIN B17 DEFINE AN ADDITIONAL CLASS OF DNA GYRASE INHIBITOR

被引：149

作者：

YORGEY, P

LEE, J

KORDEL, J

VIVAS, E

WARNER, P

JEBARATNAM, D

KOLTER, R

机构：

[1] HARVARD UNIV, SCH MED, DEPT MICROBIOL & MOLEC GENET, BOSTON, MA 02115 USA

[2] HARVARD UNIV, SCH MED, DEPT BIOL CHEM & MOLEC PHARMACOL, BOSTON, MA 02115 USA

[3] NORTHEASTERN UNIV, DEPT CHEM, BOSTON, MA 02115 USA

来源：

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 1994年 / 91卷 / 10期

关键词：

PEPTIDE ANTIBIOTICS; THIAZOLE; OXAZOLE; BLEOMYCIN;

D O I：

10.1073/pnas.91.10.4519

中图分类号：

O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

Drugs that inhibit the activity of DNA gyrase fall almost exclusively into two structural classes, the quinolones and the coumarins. A third class of DNA gyrase inhibitor is defined by the ribosomally synthesized peptide antibiotic micro cin B17 (MccB17). MccB17 contains 43 amino acid residues, but 14 of these are posttranslationally modified. Here we describe the characterization of the structure of these modifications. We propose that four cysteine and four serine side chains undergo condensation with the carbonyl group of the preceding residue, followed by alpha/beta dehydrogenation to yield four thiazole and four oxazole rings, respectively. The three proteins implicated in catalyzing these modifications (McbBCD) would constitute the only thiazole/oxazole biosynthetic enzymes identified. These results open up possibilities for the design of DNA gyrase inhibitors and add to the repertoire of posttranslational modifications with potential for protein engineering. Escherichia coli sbmA mutants, which lack the inner membrane protein (SbmA) involved in MccB17 uptake, were found to be resistant to bleomycin. Bleomycin is structurally unrelated to MccB17 except for the fact that it contains two thiazole rings. This suggests that thiazole rings are part of the MccB17 structure recognized by SbmA. This observation and the finding that SbmA homologs are widely conserved and can play developmental roles [Glazebrook, J., Ichige, A. and Walker, G. C. (1993) Genes Dev. 7, 1485-1497] suggest that thiazole- and oxazole-containing compounds may serve as signaling molecules for a wide variety of bacteria in diverse environments, including pathogen interactions with plant and animal hosts.

引用

页码：4519 / 4523

页数：5

共 27 条

[1] MICROCIN PLASMIDS - GROUP OF EXTRACHROMOSOMAL ELEMENTS CODING FOR LOW-MOLECULAR-WEIGHT ANTIBIOTICS IN ESCHERICHIA-COLI
BAQUERO, F
BOUANCHAUD, D
MARTINEZPEREZ, MC
FERNANDEZ, C
[J]. JOURNAL OF BACTERIOLOGY, 1978, 135 (02) : 342 - 347
[2] BAQUERO F, 1984, FEMS MICROBIOL LETT, V23, P117
[3] POSTTRANSLATIONAL BACKBONE MODIFICATIONS IN THE RIBOSOMAL BIOSYNTHESIS OF THE GLYCINE-RICH ANTIBIOTIC MICROCIN-B17
BAYER, A
FREUND, S
NICHOLSON, G
JUNG, G
[J]. ANGEWANDTE CHEMIE-INTERNATIONAL EDITION IN ENGLISH, 1993, 32 (09): : 1336 - 1339
[4] DNA-SEQUENCE AND MUTATIONAL ANALYSIS OF GENES INVOLVED IN THE PRODUCTION AND RESISTANCE OF THE ANTIBIOTIC PEPTIDE TRIFOLITOXIN
BREIL, BT
LUDDEN, PW
TRIPLETT, EW
[J]. JOURNAL OF BACTERIOLOGY, 1993, 175 (12) : 3693 - 3702
[5] THE CAMALEXINS - NEW PHYTOALEXINS PRODUCED IN THE LEAVES OF CAMELINA-SATIVA (CRUCIFERAE)
BROWNE, LM
CONN, KL
AYER, WA
TEWARI, JP
[J]. TETRAHEDRON, 1991, 47 (24) : 3909 - 3914
[6] PHYTOALEXINS AND THEIR ELICITORS - A DEFENSE AGAINST MICROBIAL INFECTION IN PLANTS
DARVILL, AG
ALBERSHEIM, P
[J]. ANNUAL REVIEW OF PLANT PHYSIOLOGY AND PLANT MOLECULAR BIOLOGY, 1984, 35 : 243 - 275
[7] DAVAGNINO J, 1986, Proteins Structure Function and Genetics, V1, P230, DOI 10.1002/prot.340010305
[8] THE EXPORT OF THE DNA-REPLICATION INHIBITOR MICROCIN B17 PROVIDES IMMUNITY FOR THE HOST-CELL
GARRIDO, MD
HERRERO, M
KOLTER, R
MORENO, F
[J]. EMBO JOURNAL, 1988, 7 (06) : 1853 - 1862
[9] 4-PLASMID GENES ARE REQUIRED FOR COLICIN-V SYNTHESIS, EXPORT, AND IMMUNITY
GILSON, L
MAHANTY, HK
KOLTER, R
[J]. JOURNAL OF BACTERIOLOGY, 1987, 169 (06) : 2466 - 2470
[10] A RHIZOBIUM-MELILOTI HOMOLOG OF THE ESCHERICHIA-COLI PEPTIDE ANTIBIOTIC TRANSPORT PROTEIN SBMA IS ESSENTIAL FOR BACTEROID DEVELOPMENT
GLAZEBROOK, J
ICHIGE, A
WALKER, GC
[J]. GENES & DEVELOPMENT, 1993, 7 (08) : 1485 - 1497

← 1 2 3 →