BIOMAT Database Logo BIOMAT Database Logo

Mycinamicins, new macrolide antibiotics. I. Taxonomy, production, isolation, characterization and properties. 1980

S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani

Mycinamicins, novel macrolide antibiotics were obtained from the culture broth of Micromonospora grisseorubida sp. nov. Isolation of five components, mycinamicins I, II, III, IV and V, was accomplished by silica gel adsorption or partition chromatography. Mycinsmicin I and II exhibit a strong UV absorption peak at 218 nm and have a shoulder at 240 nm. Mycinamicin III, IV and V show strong UV absorption peaks at 215 nm and around 280 nm. From their physicochemical and biological properties, the mycinamicins are classified as new macrolide antibiotics.

UI MeSH Term Description Entries
D007783 Lactones Cyclic esters of hydroxy carboxylic acids, containing a 1-oxacycloalkan-2-one structure. Large cyclic lactones of over a dozen atoms are MACROLIDES. Lactone
D008847 Micromonospora A genus of gram-positive bacteria that forms a branched mycelium. It commonly occurs as a saprophytic form in soil and aquatic environments. Micromonospora echinospora
D002627 Chemistry, Physical The study of CHEMICAL PHENOMENA and processes in terms of the underlying PHYSICAL PHENOMENA and processes. Physical Chemistry,Chemistries, Physical,Physical Chemistries
D004352 Drug Resistance, Microbial The ability of microorganisms, especially bacteria, to resist or to become tolerant to chemotherapeutic agents, antimicrobial agents, or antibiotics. This resistance may be acquired through gene mutation or foreign DNA in transmissible plasmids (R FACTORS). Antibiotic Resistance,Antibiotic Resistance, Microbial,Antimicrobial Resistance, Drug,Antimicrobial Drug Resistance,Antimicrobial Drug Resistances,Antimicrobial Resistances, Drug,Drug Antimicrobial Resistance,Drug Antimicrobial Resistances,Drug Resistances, Microbial,Resistance, Antibiotic,Resistance, Drug Antimicrobial,Resistances, Drug Antimicrobial
D000900 Anti-Bacterial Agents Substances that inhibit the growth or reproduction of BACTERIA. Anti-Bacterial Agent,Anti-Bacterial Compound,Anti-Mycobacterial Agent,Antibacterial Agent,Antibiotics,Antimycobacterial Agent,Bacteriocidal Agent,Bacteriocide,Anti-Bacterial Compounds,Anti-Mycobacterial Agents,Antibacterial Agents,Antibiotic,Antimycobacterial Agents,Bacteriocidal Agents,Bacteriocides,Agent, Anti-Bacterial,Agent, Anti-Mycobacterial,Agent, Antibacterial,Agent, Antimycobacterial,Agent, Bacteriocidal,Agents, Anti-Bacterial,Agents, Anti-Mycobacterial,Agents, Antibacterial,Agents, Antimycobacterial,Agents, Bacteriocidal,Anti Bacterial Agent,Anti Bacterial Agents,Anti Bacterial Compound,Anti Bacterial Compounds,Anti Mycobacterial Agent,Anti Mycobacterial Agents,Compound, Anti-Bacterial,Compounds, Anti-Bacterial
D001419 Bacteria One of the three domains of life (the others being Eukarya and ARCHAEA), also called Eubacteria. They are unicellular prokaryotic microorganisms which generally possess rigid cell walls, multiply by cell division, and exhibit three principal forms: round or coccal, rodlike or bacillary, and spiral or spirochetal. Bacteria can be classified by their response to OXYGEN: aerobic, anaerobic, or facultatively anaerobic; by the mode by which they obtain their energy: chemotrophy (via chemical reaction) or PHOTOTROPHY (via light reaction); for chemotrophs by their source of chemical energy: CHEMOLITHOTROPHY (from inorganic compounds) or chemoorganotrophy (from organic compounds); and by their source for CARBON; NITROGEN; etc.; HETEROTROPHY (from organic sources) or AUTOTROPHY (from CARBON DIOXIDE). They can also be classified by whether or not they stain (based on the structure of their CELL WALLS) with CRYSTAL VIOLET dye: gram-negative or gram-positive. Eubacteria
D055598 Chemical Phenomena The composition, structure, conformation, and properties of atoms and molecules, and their reaction and interaction processes. Chemical Concepts,Chemical Processes,Physical Chemistry Concepts,Physical Chemistry Processes,Physicochemical Concepts,Physicochemical Phenomena,Physicochemical Processes,Chemical Phenomenon,Chemical Process,Physical Chemistry Phenomena,Physical Chemistry Process,Physicochemical Phenomenon,Physicochemical Process,Chemical Concept,Chemistry Process, Physical,Chemistry Processes, Physical,Concept, Chemical,Concept, Physical Chemistry,Concept, Physicochemical,Concepts, Chemical,Concepts, Physical Chemistry,Concepts, Physicochemical,Phenomena, Chemical,Phenomena, Physical Chemistry,Phenomena, Physicochemical,Phenomenon, Chemical,Phenomenon, Physicochemical,Physical Chemistry Concept,Physicochemical Concept,Process, Chemical,Process, Physical Chemistry,Process, Physicochemical,Processes, Chemical,Processes, Physical Chemistry,Processes, Physicochemical
D018942 Macrolides A group of often glycosylated macrocyclic compounds formed by chain extension of multiple PROPIONATES cyclized into a large (typically 12, 14, or 16)-membered lactone. Macrolides belong to the POLYKETIDES class of natural products, and many members exhibit ANTIBIOTIC properties. Macrolide

Related Publications

S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani
Macrolide antibiotics M-4365 produced by Micromonospora. I. Taxonomy, production, isolation, characterization and properties.
June 1977, The Journal of antibiotics,
S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani
Mycinamicins, new macrolide antibiotics. XII. Isolation and structural elucidation of mycinamicins X and XI.
November 1991, The Journal of antibiotics,
S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani
Mycinamicins, new macrolide antibiotics. VIII. Chemical degradation and absolute configuration of mycinamicins.
April 1985, The Journal of antibiotics,
S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani
Mycinamicins, new macrolide antibiotics. IX. Chemical ionization mass spectral studies on mycinamicins.
July 1985, The Journal of antibiotics,
S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani
Mycinamicins, new macrolide antibiotics. IV. Structure of mycinamicin III.
March 1981, The Journal of antibiotics,
S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani
Mycinamicins, new macrolide antibiotics. III Isolation and structures of mycinamicin aglycones, mycinolide IV and V.
March 1981, The Journal of antibiotics,
S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani
Sporeamicin A, a new macrolide antibiotic. I. Taxonomy, fermentation, isolation and characterization.
May 1992, The Journal of antibiotics,
S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani
Mycinamicins, new macrolide antibiotics. XI. Isolation and structure elucidation of a key intermediate in the biosynthesis of the mycinamicins, mycinamicin VIII.
December 1989, The Journal of antibiotics,
S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani
YS-822A, a new polyene macrolide antibiotic. I. Production, isolation, characterization and biological properties.
August 1990, The Journal of antibiotics,
S Satoi, and N Muto, and M Hayashi, and T Fujii, and M Otani
Mycinamicins, new macrolide antibiotics. V. Isolation and structures of new 16-membered aglycones, mycinolide IV and protomycinolide IV.
August 1981, The Journal of antibiotics,
Copied contents to your clipboard!