Genomic and structural basis for evolution of tropane alkaloid biosynthesis

The tropane alkaloids (TAs) cocaine and hyoscyamine have been used medicinally for thousands of years. To understand the evolutionary origins and trajectories of serial biosynthetic enzymes of TAs and especially the characteristic tropane skeletons, we generated the chromosome-level genome assemblie...

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Published inProceedings of the National Academy of Sciences - PNAS Vol. 120; no. 17; p. e2302448120
Main Authors Wang, Yong-Jiang, Tain, Tian, Yu, Jia-Yi, Li, Jie, Xu, Bingyan, Chen, Jianghua, D'Auria, John C, Huang, Jian-Ping, Huang, Sheng-Xiong
Format Journal Article
LanguageEnglish
Published United States National Academy of Sciences 25.04.2023
Subjects
Alkaloids
Biological evolution
Biological Sciences
Biosynthesis
Chromosomes
Cocaine
Divergence
Enzymes
Erythroxylaceae
Evolution
Genomic analysis
Genomics
Hyoscyamine
Methyltransferases - genetics
Molecular docking
Molecular Docking Simulation
Mutation
N-Methyltransferase
Origins
Phylogeny
Polyamines
Putrescine
Salicylic acid
Salicylic acid methyltransferase
Solanaceae
Solanaceae - genetics
Spermidine
Spermidine synthase
Substrates
Synteny
Tropane alkaloids
Tropanes
genome
tropane alkaloids
structural biology
evolution
biosynthesis
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Summary:The tropane alkaloids (TAs) cocaine and hyoscyamine have been used medicinally for thousands of years. To understand the evolutionary origins and trajectories of serial biosynthetic enzymes of TAs and especially the characteristic tropane skeletons, we generated the chromosome-level genome assemblies of cocaine-producing (Erythroxylaceae, rosids clade) and hyoscyamine-producing (Solanaceae, asterids clade). Comparative genomic and phylogenetic analysis suggested that the lack of spermidine synthase/ -methyltransferase ( SPMT1) in ancestral asterids species contributed to the divergence of polyamine (spermidine or putrescine) methylation in cocaine and hyoscyamine biosynthesis. Molecular docking analysis and key site mutation experiments suggested that ecgonone synthases CYP81AN15 and CYP82M3 adopt different active-site architectures to biosynthesize the same product ecgonone from the same substrate in Erythroxylaceae and Solanaceae. Further synteny analysis showed different evolutionary origins and trajectories of CYP81AN15 and CYP82M3, particularly the emergence of through the neofunctionalization of ancient tandem duplication genes. The combination of structural biology and comparative genomic analysis revealed that ecgonone methyltransferase, which is responsible for the biosynthesis of characteristic 2-substituted carboxymethyl group in cocaine, evolved from the tandem copies of salicylic acid methyltransferase by the mutations of critical E216 and S153 residues. Overall, we provided strong evidence for the independent origins of serial TA biosynthetic enzymes on the genomic and structural level, underlying the chemotypic convergence of TAs in phylogenetically distant species.
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Edited by Ian Baldwin, Max-Planck-Institut fur chemische Okologie Abteilung fur Molekulare Okologie, Jena, Germany; received February 12, 2023; accepted March 23, 2023
1Y.-J.W., T.T., and J.-Y.Y. contributed equally to this work.
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.2302448120