Antimicrobial activities of chemically modified thiazolyl peptide antibiotic MDL 62,879 (GE2270A)

被引：11

作者：

Lociuro, S ^{[1
]}

Tavecchia, P ^{[1
]}

Marzorati, E ^{[1
]}

Landini, P ^{[1
]}

Goldstein, BP ^{[1
]}

Denaro, M ^{[1
]}

Ciabatti, R ^{[1
]}

机构：

[1] BIOSEARCH ITALIA SPA, I-21040 GERENZANO, VA, ITALY

来源：

JOURNAL OF ANTIBIOTICS | 1997年 / 50卷 / 04期

关键词：

D O I：

10.7164/antibiotics.50.344

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：

MDL 62,879 (GE2270A) 1 is a new inhibitor of elongation factor-Tu (EF-Tu) and belongs to the class of thiazolyl peptide antibiotics. Controlled acid hydrolysis of 1 followed by treatment with base resulted in the lost of the two terminal amino acids and in the formation of water-soluble MDL 62,935 2. Although less active in vitro than its parent compound, 2 was able to inhibit by 50% an Escherichia coli cell-free protein synthesis system at roughly the same concentration of 1. MDL 63,935 2 was subjected to further modification at the beta-phenylserine residue. Derivatives obtained from 2 were less active in both antimicrobial (MIC) and enzymatic (IC50) assays. This suggests that beta-phenylserine plays an important role for the inhibition of EF-Tu by 1 and 2.

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页码：344 / 349

页数：6

相关论文

共 16 条

[1] NEW ANTIBIOTIC THAT ACTS SPECIFICALLY ON THE GTP-BOUND FORM OF ELONGATION FACTOR-TU [J].

ANBORGH, PH ;

PARMEGGIANI, A .

EMBO JOURNAL, 1991, 10 (04) :779-784

[2]

BERTI M, 1992, INT J MED MICROBIO S, V22, P442

[3] INVITRO ANTIMICROBIAL ACTIVITY OF A NEW ANTIBIOTIC, MDL-62,879 (GE2270-A) [J].

GOLDSTEIN, BP ;

BERTI, M ;

RIPAMONTI, F ;

RESCONI, A ;

SCOTTI, R ;

DENARO, M .

ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1993, 37 (04) :741-745

[4] INVITRO ACTIVITY OF MDL-62,879 (GE2270-A) AGAINST AEROBIC GRAM-POSITIVE AND ANAEROBIC-BACTERIA [J].

KING, A ;

BETHUNE, L ;

PHILLIPS, I .

ANTIMICROBIAL AGENTS AND CHEMOTHERAPY, 1993, 37 (04) :746-749

[5] SENSITIVITY OF ELONGATION-FACTOR TU (EF-TU) FROM DIFFERENT BACTERIAL SPECIES TO THE ANTIBIOTICS EFROTOMYCIN, PULVOMYCIN AND MDL-62879 [J].

LANDINI, P ;

BANDERA, M ;

SOFFIENTINI, A ;

GOLDSTEIN, BP .

JOURNAL OF GENERAL MICROBIOLOGY, 1993, 139 :769-774

[6] INHIBITION OF BACTERIAL PROTEIN-SYNTHESIS BY ELONGATION-FACTOR-TO-BINDING ANTIBIOTICS MDL-62,879 AND EFROTOMYCIN [J].

LANDINI, P ;

BANDERA, M ;

GOLDSTEIN, BP ;

RIPAMONTI, F ;

SOFFIENTINI, A ;

ISLAM, K ;

DENARO, M .

BIOCHEMICAL JOURNAL, 1992, 283 :649-652

[7] MECHANISM OF ACTION OF KIRROMYCIN-LIKE ANTIBIOTICS [J].

PARMEGGIANI, A ;

SWART, GWM .

ANNUAL REVIEW OF MICROBIOLOGY, 1985, 39 :557-577

[8] ANTIBIOTIC GE2270-A - A NOVEL INHIBITOR OF BACTERIAL PROTEIN-SYNTHESIS .1. ISOLATION AND CHARACTERIZATION [J].

SELVA, E ;

BERETTA, G ;

MONTANINI, N ;

SADDLER, GS ;

GASTALDO, L ;

FERRARI, P ;

LORENZETTI, R ;

LANDINI, P ;

RIPAMONTI, F ;

GOLDSTEIN, BP ;

BERTI, M ;

MONTANARO, L ;

DENARO, M .

JOURNAL OF ANTIBIOTICS, 1991, 44 (07) :693-701

[9] NOVEL ANTIBIOTICS, AMYTHIAMICINS .3. STRUCTURE ELUCIDATIONS OF AMYTHIAMICIN-A, AMYTHIAMICIN-B AND AMYTHIAMICIN-C [J].

SHIMANAKA, K ;

TAKAHASHI, Y ;

IINUMA, H ;

NAGANAWA, H ;

TAKEUCHI, T .

JOURNAL OF ANTIBIOTICS, 1994, 47 (10) :1153-1159

[10] NOVEL ANTIBIOTICS, AMYTHIAMICINS .4. A MUTATION IN THE ELONGATION-FACTOR TU GENE IN A RESISTANT MUTANT OF BACILLUS-SUBTILIS [J].

SHIMANAKA, K ;

IINUMA, H ;

HAMADA, M ;

IKENO, S ;

TSUCHIYA, KS ;

ARITA, M ;

HORI, M .

JOURNAL OF ANTIBIOTICS, 1995, 48 (02) :182-184