PERFORM Publications

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Title		Authors	PubMed ID
1	Benzylisoquinoline Alkaloid Production in Yeast via Norlaudanosoline Improves Titer, Selectivity, and Yield	Narcross L; Pyne ME; Kevvai K; Siu KH; Dueber JE; Martin VJJ;	41779670 BIOLOGY
2	A Highly Characterized Synthetic Landing Pad System for Precise Multicopy Gene Integration in Yeast.	Bourgeois L, Pyne ME, Martin VJJ	30372609 BIOLOGY
3	Microbial Factories for the Production of Benzylisoquinoline Alkaloids.	Narcross L, Fossati E, Bourgeois L, Dueber JE, Martin VJJ	26775900 BIOLOGY
4	Engineering of a Nepetalactol-Producing Platform Strain of Saccharomyces cerevisiae for the Production of Plant Seco-Iridoids.	Campbell A, Bauchart P, Gold ND, Zhu Y, De Luca V, Martin VJ	26981892 CSFG
5	Reconstituting Plant Secondary Metabolism in Saccharomyces cerevisiae for Production of High-Value Benzylisoquinoline Alkaloids.	Pyne ME, Narcross L, Fossati E, Bourgeois L, Burton E, Gold ND, Martin VJ	27417930 CSFG
6	Mining Enzyme Diversity of Transcriptome Libraries through DNA Synthesis for Benzylisoquinoline Alkaloid Pathway Optimization in Yeast.	Narcross L, Bourgeois L, Fossati E, Burton E, Martin VJ	27442619 BIOLOGY

Title:	Mining Enzyme Diversity of Transcriptome Libraries through DNA Synthesis for Benzylisoquinoline Alkaloid Pathway Optimization in Yeast.
Authors:	Narcross L, Bourgeois L, Fossati E, Burton E, Martin VJ
Link:	https://www.ncbi.nlm.nih.gov/pubmed/27442619?dopt=Abstract
DOI:	10.1021/acssynbio.6b00119
Publication:	ACS synthetic biology
Keywords:	Saccharomyces cerevisiae; benzylisoquinoline alkaloids; dihydrosanguinarine; pathway optimization; synthetic DNA; transcriptome mining;
PMID:	27442619	Category:	ACS Synth Biol	Date Added:	2019-06-07
Dept Affiliation:	BIOLOGY 1 Department of Biology, Concordia University , Montréal, Québec H4B 1R6, Canada. 2 Centre for Structural and Functional Genomics, Concordia University , Montréal, Québec H4B 1R6, Canada.

Description:

Mining Enzyme Diversity of Transcriptome Libraries through DNA Synthesis for Benzylisoquinoline Alkaloid Pathway Optimization in Yeast.

ACS Synth Biol. 2016 12 16;5(12):1505-1518

Authors: Narcross L, Bourgeois L, Fossati E, Burton E, Martin VJ

Abstract

The ever-increasing quantity of data deposited to GenBank is a valuable resource for mining new enzyme activities. Falling costs of DNA synthesis enables metabolic engineers to take advantage of this resource for identifying superior or novel enzymes for pathway optimization. Previously, we reported synthesis of the benzylisoquinoline alkaloid dihydrosanguinarine in yeast from norlaudanosoline at a molar conversion of 1.5%. Molar conversion could be improved by reduction of the side-product N-methylcheilanthifoline, a key bottleneck in dihydrosanguinarine biosynthesis. Two pathway enzymes, an N-methyltransferase and a cytochrome P450 of the CYP719A subfamily, were implicated in the synthesis of the side-product. Here, we conducted an extensive screen to identify enzyme homologues whose coexpression reduces side-product synthesis. Phylogenetic trees were generated from multiple sources of sequence data to identify a library of candidate enzymes that were purchased codon-optimized and precloned into expression vectors designed to facilitate high-throughput analysis of gene expression as well as activity assay. Simple in vivo assays were sufficient to guide the selection of superior enzyme homologues that ablated the synthesis of the side-product, and improved molar conversion of norlaudanosoline to dihydrosanguinarine to 10%.

PMID: 27442619 [PubMed - indexed for MEDLINE]

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