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High-quality genome assembly and multi-omics analysis of pigment synthesis pathway in . | LitMetric

High-quality genome assembly and multi-omics analysis of pigment synthesis pathway in .

Front Microbiol

Lab of Genetic Breeding of Edible Fungi, Horticultural, College of Horticulture, Jilin Agricultural University, Changchun, China.

Published: June 2023

Owing to its great market potential for food and health care, white , a rare edible fungus, has received increased attention in recent years. This study presents a high-quality genome assembly of and multi-omics analysis of its pigment synthesis pathway. Continuous Long Reads libraries, combined with Hi-C-assisted assembly were used to assemble of white . Based on this data, we analyzed the transcriptome and metabolome of purple and white strains during the mycelium, primordium, and fruiting body stages. Finally, we obtained the genome of assembled from 13 clusters. Comparative and evolutionary analysis suggests that is more closely related to than to . The divergence of white/purple occurred approximately 40,000 years ago, and there were numerous inversions and translocations between homologous regions of the two genomes. Purple strain synthesized pigment via the shikimate pathway. The pigment in the fruiting body of was γ-glutaminyl-3,4-dihydroxy-benzoate. During pigment synthesis, α-D-glucose-1P, citrate, 2-Oxoglutarate, and glutamate were four important intermediate metabolites, whereas polyphenol oxidase and other 20 enzyme genes were the key enzymes. This study sheds light on the genetic blueprint and evolutionary history of the white genome, revealing the mechanism of pigment synthesis in . It has important theoretical and practical implications for understanding the evolution of basidiomycetes, molecular breeding of white , and deciphering the genetic regulations of edible fungi. Additionally, it provides valuable insights for the study of phenotypic traits in other edible fungi.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10308021PMC
http://dx.doi.org/10.3389/fmicb.2023.1211795DOI Listing

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