Identification of the Cytochrome P450 Monooxygenase that Bridges the Clavine and Ergoline Alkaloid Pathways

Clavines and D ‐lysergic acid‐derived alkaloid amides and alkaloid peptides are two different families of compounds that have the indole‐derived tetracyclic metergoline ring system in common. Previous work has shown that D ‐lysergic acid is biosynthetically derived from clavine alkaloids. Recent cloning and analysis of the ergot alkaloid biosynthesis gene cluster from the D ‐lysergic acid peptide (ergopeptines)‐producing Claviceps purpurea , has shown that it most probably contains all genes necessary for D ‐lysergic acid synthesis as well as those that encode the assembly of D ‐lysergic acid peptides, such as ergotamine. To address the role of the oxygenase genes of alkaloid‐gene clusters, the only cytochrome P450 monooxygenase gene of this cluster was inactivated by disruption. The resultant mutant accumulated agroclavine, elymoclavine, and chanoclavine in substantial amounts but not ergopeptines. Feeding the mutant with D ‐lysergic acid restored ergopeptine synthesis; this suggests a block in the conversion of elymoclavine to D ‐lysergic acid. The gene was designated cloA (for encoding a cl avine o xidase, CLOA). Retransformation of the mutant with the intact cloA gene also restored ergopeptine synthesis. These data show that CLOA catalyses the conversion of clavines to D ‐lysergic acid, it acts as a critical enzyme in the ergot alkaloid gene cluster, and bridges the biosynthesis of the two different families of alkaloids.