| Literature DB >> 25228340 |
Matthew A Bedewitz1, Elsa Góngora-Castillo2, Joseph B Uebler1, Eliana Gonzales-Vigil1, Krystle E Wiegert-Rininger1, Kevin L Childs2, John P Hamilton2, Brieanne Vaillancourt2, Yun-Soo Yeo3, Joseph Chappell3, Dean DellaPenna4, A Daniel Jones5, C Robin Buell2, Cornelius S Barry6.
Abstract
The tropane alkaloids, hyoscyamine and scopolamine, are medicinal compounds that are the active components of several therapeutics. Hyoscyamine and scopolamine are synthesized in the roots of specific genera of the Solanaceae in a multistep pathway that is only partially elucidated. To facilitate greater understanding of tropane alkaloid biosynthesis, a de novo transcriptome assembly was developed for Deadly Nightshade (Atropa belladonna). Littorine is a key intermediate in hyoscyamine and scopolamine biosynthesis that is produced by the condensation of tropine and phenyllactic acid. Phenyllactic acid is derived from phenylalanine via its transamination to phenylpyruvate, and mining of the transcriptome identified a phylogenetically distinct aromatic amino acid aminotransferase (ArAT), designated Ab-ArAT4, that is coexpressed with known tropane alkaloid biosynthesis genes in the roots of A. belladonna. Silencing of Ab-ArAT4 disrupted synthesis of hyoscyamine and scopolamine through reduction of phenyllactic acid levels. Recombinant Ab-ArAT4 preferentially catalyzes the first step in phenyllactic acid synthesis, the transamination of phenylalanine to phenylpyruvate. However, rather than utilizing the typical keto-acid cosubstrates, 2-oxoglutarate, pyruvate, and oxaloacetate, Ab-ArAT4 possesses strong substrate preference and highest activity with the aromatic keto-acid, 4-hydroxyphenylpyruvate. Thus, Ab-ArAT4 operates at the interface between primary and specialized metabolism, contributing to both tropane alkaloid biosynthesis and the direct conversion of phenylalanine to tyrosine.Entities:
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Year: 2014 PMID: 25228340 PMCID: PMC4213168 DOI: 10.1105/tpc.114.130534
Source DB: PubMed Journal: Plant Cell ISSN: 1040-4651 Impact factor: 11.277