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  2. New antitumor antibiotic, LL-D05139 beta. Fermentation, isolation, structure determination and biological activities

New antitumor antibiotic, LL-D05139 beta. Fermentation, isolation, structure determination and biological activities

  • J Antibiot (Tokyo). 1987 Dec;40(12):1657-63. doi: 10.7164/antibiotics.40.1657.
M D Lee 1 A A Fantini N A Kuck M Greenstein R T Testa D B Borders
Affiliations

Affiliation

  • 1 American Cyanamid Co., Medical Research Division, Lederle Laboratories, Pearl River, New York 10965.
Abstract

The LL-D05139 complex, containing LL-D05139 beta and azaserine, was recovered from the fermentation filtrate of Glycomyces harbinensis (NRRL 15337). A chemically defined medium was developed which favored the production of LL-D05139 beta. Antibiotic LL-D05139 beta was isolated from the fermentation filtrate by adsorption on granular carbon and further purified by chromatography on microcrystalline cellulose. Acid hydrolysis of LL-D05139 beta gave one molar equivalent each of alanine and serine. Both Amino acids were found to have the L-configuration by GC analysis on a chiral column and alanine was assigned to be the N-terminal amino acid by Edman degradation. This information coupled with IR, UV, 1H NMR, 13C NMR and MS spectral data allowed us to assign the structure of LL-D05139 beta as alanylazaserine. LL-D05139 beta demonstrated greater Antibacterial and biochemical induction assay activities than azaserine. The two drugs showed similar antitumor activities.

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