Author:
McFarland J W,Pirie D K,Retsema J A,English A R
Abstract
Novel N-acyl analogs of lankacidin may be prepared from 3-isocyanatolankone diformate [7,13-bis(formyloxy)-2-isocyanato-1,4,10,19-tetramethyl-16- oxabicyclo[13.2.2.]nonadeca-3,5,9,11-tetraen-17,18-dione]. Of seven such analogs evaluated in vitro only homolankacidin diformate showed significant activity. However, in a cell-free system two of the inactive analogs inhibited polypeptide synthesis as well as did lankacidin itself or erythromycin. Antibacterial activity, therefore, is a function of the ability of a congener to penetrate the bacterial cell membrane in addition to its intrinsic activity. Similarly, lankacidinol is as potent as lankacidin or erythromycin as an inhibitor of bacterial polypeptide synthesis in a cell-free system. This intrinsic activity is expressed as potent antibacterial activity against growing gram-positive cultures in O(2')-acyl derivatives with the proper lipophilicity.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Pharmacology (medical),Pharmacology
Reference19 articles.
1. Zersetzung von N-Monosubstituierten Carbaminsaure-carbonsaure-anhydriden;Babusiaux P.;Justus Liebigs Ann. Chem.,1976
2. Evaluation of three 4"-deoxy-4;English A. R.;Antimicrob. Agents Chemother.,1984
3. Studies on T-2636 antibiotics. III. A new component, T-2636F;Fugono T.;J. Antibiot.,1971
4. Interconversion of T-2636 antibiotics produced by Streptomyces rochei var. volubilis;Fugono T.;Experientia,1970
5. Stoffwechselprodukte in Actinomyceten;Gaumann E.;Lankamycin und Lankacidin. Helv. Chim. Acta,1960
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