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Novel avilamycin derivatives with improved polarity generated by targeted gene disruption
Authors:Weitnauer Gabriele  Hauser Gerd  Hofmann Carsten  Linder Ulrike  Boll Raija  Pelz Klaus  Glaser Steffen J  Bechthold Andreas
Affiliation:Pharmazeutische Biologie und Biotechnologie, Institut für Pharmazeutische Wissenschaften, Albert-Ludwigs-Universit?t Freiburg, Stefan-Meier-Strasse 19, 79104 Freiburg, Germany.
Abstract:The oligosaccharide antibiotics avilamycin A and C are produced by Streptomyces viridochromogenes Tu57. Both consist of a heptasaccharide chain, which is attached to a polyketide-derived dichloroisoeverninic acid moiety. They show excellent antibiotic activity against Gram-positive bacteria. Both molecules are modified by O-methylation at different positions, which contributes to poor water solubility and difficulties in galenical drug development. In order to generate novel avilamycin derivatives with improved polarity and improved pharmacokinetic properties, we generated a series of mutants with one, two, or three mutated methyltransferase genes. Based on the structure of the novel avilamycin derivatives, the exact function of three methyltransferases, AviG2, AviG5, and AviG6, involved in avilamycin biosynthesis could be assigned.
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