4.7 Article

Prospecting Biotechnologically-Relevant Monooxygenases from Cold Sediment Metagenomes: An In Silico Approach

期刊

MARINE DRUGS
卷 15, 期 4, 页码 -

出版社

MDPI
DOI: 10.3390/md15040114

关键词

bacterial cytochrome P450; Baeyer-Villiger monooxygenases; bioprospecting biocatalysts; phylogenetic analysis; molecular modeling

资金

  1. Department of Energy-Joint Genome Institute (DOE-JGI) under the Community Sequencing Program (CSP) [328, 403959, 404206, 404777-404782, 404786, 404788-404801]
  2. CONICET (PIP) [11220130100174]
  3. National Agency for the Promotion of Science and Technology of Argentina (ANPCyT PICT) [2102]
  4. grants CONICET PIP [11220110101156, 11220150100934CO, UNR BIO287, BIO451]
  5. University of Buenos Aires [UBA 2014-2017 20020130100569BA]
  6. European Commission through the Marie Curie Action IRSES
  7. IMCONet (International Research Staff Exchange Scheme
  8. Interdisciplinary Modelling of Climate Change in Coastal Western Antarctica-Network for Staff Exchange and Training) [318718]
  9. Argentinean Antarctic Institute
  10. Argentinean Antarctic Institute (PICTO) [0124]
  11. Pacific Northwest National Laboratory [DE-AC05-76RLO1830]
  12. Research Council of Norway [228107]

向作者/读者索取更多资源

The goal of this work was to identify sequences encoding monooxygenase biocatalysts with novel features by in silico mining an assembled metagenomic dataset of polar and subpolar marine sediments. The targeted enzyme sequences were Baeyer-Villiger and bacterial cytochrome P450 monooxygenases (CYP153). These enzymes have wide-ranging applications, from the synthesis of steroids, antibiotics, mycotoxins and pheromones to the synthesis of monomers for polymerization and anticancer precursors, due to their extraordinary enantio-, regio-, and chemo-selectivity that are valuable features for organic synthesis. Phylogenetic analyses were used to select the most divergent sequences affiliated to these enzyme families among the 264 putative monooxygenases recovered from the similar to 14 million protein-coding sequences in the assembled metagenome dataset. Three-dimensional structure modeling and docking analysis suggested features useful in biotechnological applications in five metagenomic sequences, such as wide substrate range, novel substrate specificity or regioselectivity. Further analysis revealed structural features associated with psychrophilic enzymes, such as broader substrate accessibility, larger catalytic pockets or low domain interactions, suggesting that they could be applied in biooxidations at room or low temperatures, saving costs inherent to energy consumption. This work allowed the identification of putative enzyme candidates with promising features from metagenomes, providing a suitable starting point for further developments.

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