Natural Variation in the Microcystin Synthetase Operon mcyABC and Impact on Microcystin Production in Microcystis Strains

Author:

Mikalsen Bjørg1,Boison Gudrun2,Skulberg Olav M.3,Fastner Jutta4,Davies William1,Gabrielsen Tove M.1,Rudi Knut5,Jakobsen Kjetill S.1

Affiliation:

1. Department of Biology, University of Oslo, 0315 Oslo

2. Institute of Botany, University of Cologne, D-50923 Cologne

3. NIVA, Norwegian Institute for Water Research, 0411 Oslo

4. Technical University of Berlin, 10587 Berlin, Germany

5. MATFORSK, Norwegian Food Research Institute, 1430 Ås, Norway

Abstract

ABSTRACT Toxic Microcystis strains often produce several isoforms of the cyclic hepatotoxin microcystin, and more than 65 isoforms are known. This has been attributed to relaxed substrate specificity of the adenylation domain. Our results show that in addition to this, variability is also caused by genetic variation in the microcystin synthetase genes. Genetic characterization of a region of the adenylation domain in module mcyB1 resulted in identification of two groups of genetic variants in closely related Microcystis strains. Sequence analyses suggested that the genetic variation is due to recombination events between mcyB1 and the corresponding domains in mcyC . Each variant could be correlated to a particular microcystin isoform profile, as identified by matrix-assisted laser desorption ionization-time of flight mass spectrometry. Among the Microcystis species studied, we found 11 strains containing different variants of the mcyABC gene cluster and 7 strains lacking the genes. Furthermore, there is no concordance between the phylogenies generated with mcyB1 , 16S ribosomal DNA, and DNA fingerprinting. Collectively, these results suggest that recombination between imperfect repeats, gene loss, and horizontal gene transfer can explain the distribution and variation within the mcyABC operon.

Publisher

American Society for Microbiology

Subject

Molecular Biology,Microbiology

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