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PLANT BIOLOGY
A gene cluster for secondary metabolism in oat: Implications for the evolution of metabolic diversity in plants



*Sainsbury Laboratory, John Innes Centre, Norwich NR4 7UH, United Kingdom;
Institute of Grassland and Environmental Research, Plas Gogerddan, Aberystwyth SY23 3EB, Wales, United Kingdom; and
DuPont Agricultural Products, P.O. Box 80402, Wilmington, DE 19880
Edited by Meinhart H. Zenk, University of Halle, Halle/Saale, Germany, and approved April 13, 2004 (received for review February 24, 2004)
The evolution of the ability to synthesize specialized metabolites is likely to have been key for survival and diversification of different plant species. Oats (Avena spp.) produce antimicrobial triterpenoids (avenacins) that protect against disease. The oat
-amyrin synthase gene AsbAS1, which encodes the first committed enzyme in the avenacin biosynthetic pathway, is clearly distinct from other plant
-amyrin synthases. Here we show that AsbAS1 has arisen by duplication and divergence of a cycloartenol synthase-like gene, and that its properties have been refined since the divergence of oats and wheat. Strikingly, we have also found that AsbAS1 is clustered with other genes required for distinct steps in avenacin biosynthesis in a region of the genome that is not conserved in other cereals. Because the components of this gene cluster are required for at least four clearly distinct enzymatic processes (2,3-oxidosqualene cyclization,
-amyrin oxidation, glycosylation, and acylation), it is unlikely that the cluster has arisen as a consequence of duplication of a common ancestor. Although clusters of paralogous genes are common in plants (e.g., gene clusters for rRNA and specific disease resistance), reports of clusters of genes that do not share sequence relatedness and whose products contribute to a single selectable function are rare [Gierl, A. & Frey, M. (2001) Planta 213, 493498]. Taken together, our evidence has important implications for the generation of metabolic diversity in plants.
Abbreviation: cM, centimorgan.
To whom correspondence should be addressed. E-mail: annie.osbourn{at}sainsbury-laboratory.ac.uk.
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